ENSPRYNG is indicated for the treatment of neuromyelitis optica spectrum disorder (NMOSD) in adult patients who are anti-aquaporin-4 (AQP4) antibody positive.

{ "type": "p", "children": [], "text": "ENSPRYNG is indicated for the treatment of neuromyelitis optica spectrum disorder (NMOSD) in adult patients who are anti-aquaporin-4 (AQP4) antibody positive." }

Hepatitis B Virus Screening

Prior to initiating ENSPRYNG, perform Hepatitis B virus (HBV) screening. ENSPRYNG is contraindicated in patients with active HBV confirmed by positive results for surface antigen [HBsAg] and anti-HBV tests. For patients who are negative for HBsAg and positive for HB core antibody [HBcAb+] or are carriers of HBV [HBsAg+], consult liver disease experts before starting and during treatment with ENSPRYNG [see Contraindications (4) and Warnings and Precautions (5.1)].

Tuberculosis Screening

Prior to initiating ENSPRYNG, evaluate for active tuberculosis and test for latent infection. For patients with active tuberculosis or positive tuberculosis screening without a history of appropriate treatment, consult infectious disease experts before initiating treatment with ENSPRYNG [see Contraindications (4) and Warnings and Precautions (5.1)].

Liver Transaminase Screening

Liver transaminases and serum bilirubin should be assessed prior to initiation of treatment with ENSPRYNG [see Warnings and Precautions (5.2)].

Caution should be exercised when considering initiation of ENSPRYNG treatment in patients whose aspartate aminotransferase (AST) or alanine aminotransferase (ALT) levels are greater than 1.5 times the upper limit of normal (ULN).

Vaccinations

Because vaccination with live-attenuated or live vaccines is not recommended during treatment with ENSPRYNG, administer all immunizations according to immunization guidelines at least 4 weeks prior to initiation of ENSPRYNG for live or live-attenuated vaccines and, whenever possible, at least 2 weeks prior to initiation of ENSPRYNG for non-live vaccines [see Warnings and Precautions (5.1)].

For subcutaneous use only.

Prior to every use of ENSPRYNG, advise patients to consult with their healthcare professional (HCP) if they suspect an active infection, including localized infections. In case of active infection, delay use of ENSPRYNG until the infection is resolved [see Warnings and Precautions (5.1)].

The recommended loading dosage of ENSPRYNG for the first three administrations is 120 mg by subcutaneous injection at Weeks 0, 2, and 4, followed by a maintenance dosage of 120 mg every 4 weeks.

Missed Dose

If a dose of ENSPRYNG is missed for any reason other than increases in liver enzymes [see Dosage and Administration (2.4)], administer as described in Table 1.

<div class="scrollingtable"><table width="75%"> <caption> <span>Table 1 Recommended Dosage for Delayed or Missed Doses</span> </caption> <col align="left" valign="top" width="35%"/> <col align="left" valign="top" width="65%"/> <thead> <tr class="First Last"> <th align="left" class="Lrule Rrule">Last Dose Administered</th><th align="left" class="Rrule">Recommended Dosage for Delayed or Missed Doses</th> </tr> </thead> <tfoot> <tr> <td align="left" colspan="2"> <dl class="Footnote"> <dt> <a href="#footnote-reference-1" name="footnote-1">*</a> </dt> <dd>"0 weeks" refers to time of the first administration after the missed dose.</dd> </dl> </td> </tr> </tfoot> <tbody> <tr class="Botrule First"> <td align="left" class="Lrule Rrule">Less than 8 weeks during the maintenance period or missed a loading dose</td><td align="left" class="Rrule">Administer 120 mg by subcutaneous injection as soon as possible, and do not wait until the next planned dose.<br/> <span class="Underline">Maintenance period</span> <br/>After the delayed or missed dose is administered, reset the dose schedule to every 4 weeks.<br/> <span class="Underline">Loading period</span> <br/>If the second loading dose is delayed or missed, administer as soon as possible and administer the 3<span class="Sup">rd</span> and final loading dose 2 weeks later.<br/>If the third loading dose is delayed or missed, administer as soon as possible and administer the 1<span class="Sup">st</span> maintenance dose 4 weeks later.</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">8 weeks to less than 12 weeks</td><td align="left" class="Rrule">120 mg by subcutaneous injection at 0<a class="Sup" href="#footnote-1" name="footnote-reference-1">*</a> and 2 weeks, followed by 120 mg every 4 weeks.</td> </tr> <tr class="Last"> <td align="left" class="Lrule Rrule">12 weeks or longer</td><td align="left" class="Rrule">120 mg by subcutaneous injection at 0<a class="Sup" href="#footnote-1">*</a>, 2, and 4 weeks followed by 120 mg every 4 weeks.</td> </tr> </tbody> </table></div>

Liver Transaminases

Monitor ALT and AST levels every 4 weeks for the first 3 months of treatment with ENSPRYNG, followed by every 3 months for one year, and thereafter as clinically necessary [see Warnings and Precautions (5.2)].

If an ALT or AST elevation of greater than 5 times the ULN occurs, discontinue ENSPRYNG as follows:

Neutrophil Counts

Monitor neutrophils 4 to 8 weeks after initiation of therapy and thereafter at regular clinically determined intervals. If the neutrophil count is below 1.0 × 109/L and confirmed by repeat testing, ENSPRYNG should be interrupted until the neutrophil count is > 1.0 × 109/L [see Warnings and Precautions (5.3)].

Injection: 120 mg/mL clear, and colorless to slightly yellow solution in single-dose prefilled syringe.

{ "type": "p", "children": [], "text": "Injection: 120 mg/mL clear, and colorless to slightly yellow solution in single-dose prefilled syringe." }

ENSPRYNG is contraindicated in patients with:

{ "type": "p", "children": [], "text": "ENSPRYNG is contraindicated in patients with:" }

{ "type": "ul", "children": [ "A known hypersensitivity to satralizumab or any of the inactive ingredients [see Warnings and Precautions (5.4)]\n", "Active Hepatitis B infection [see Warnings and Precautions (5.1)]\n", "Active or untreated latent tuberculosis [see Warnings and Precautions (5.1)]\n" ], "text": "" }

An increased risk of infections, including serious and potentially fatal infections, has been observed in patients treated with IL-6 receptor antagonists, including ENSPRYNG.

The most common infections reported in a randomized clinical trial of patients treated with ENSPRYNG who were not on other chronic immunosuppressant therapies (Study 1), and that occurred more often than in patients receiving placebo, were nasopharyngitis (12%) and cellulitis (10%). The most common infections in patients who were on an additional concurrent immunosuppressant, and that occurred more often than in patients receiving placebo, were nasopharyngitis (31%), upper respiratory infection (19%), and pharyngitis (12%).

Delay ENSPRYNG administration in patients with an active infection, including localized infections, until the infection is resolved.

Hepatitis B Virus (HBV) Reactivation

Risk of HBV reactivation has been observed with other immunosuppressant therapies. Patients with chronic HBV infection were excluded from clinical trials. Perform HBV screening in all patients before initiation of treatment with ENSPRYNG. Do not administer ENSPRYNG to patients with active hepatitis. For patients who are chronic carriers of HBV [HBsAg+] or are negative for HBsAg and positive for HB core antibody [HBcAb+], consult liver disease experts before starting and during treatment with ENSPRYNG.

Tuberculosis

Tuberculosis has occurred in patients treated with other interleukin-6 receptor antagonists. Patients should be evaluated for tuberculosis risk factors and tested for latent infection prior to initiating ENSPRYNG. Consider anti-tuberculosis therapy prior to initiation of ENSPRYNG in patients with a history of latent or active tuberculosis in whom an adequate course of treatment cannot be confirmed, and for patients with a negative test for latent tuberculosis but having risk factors for tuberculosis infection. Consult infectious disease experts regarding whether initiating anti-tuberculosis therapy is appropriate before starting treatment. Patients should be monitored for the development of symptoms and signs of tuberculosis with ENSPRYNG, even if initial tuberculosis testing is negative.

Vaccinations

Live or live-attenuated vaccines should not be given concurrently with ENSPRYNG because clinical safety has not been established. Administer all immunizations according to immunization guidelines at least 4 weeks prior to initiation of ENSPRYNG for live or live-attenuated vaccines and, whenever possible, at least 2 weeks prior to initiation of ENSPRYNG for non-live vaccines.

Mild and moderate elevations of liver enzymes have been observed in patients treated with ENSPRYNG at a higher incidence than in patients receiving placebo [see Adverse Reactions (6.1)].

ALT and AST levels should be monitored every 4 weeks for the first 3 months of treatment, followed by every 3 months for one year, and thereafter, as clinically indicated [see Dosage and Administration (2.4)].

Decreases in neutrophil counts were observed in patients treated with ENSPRYNG at a higher incidence than placebo [see Adverse Reactions (6.1)].

Neutrophil counts should be monitored 4 to 8 weeks after initiation of therapy, and thereafter at regular clinically determined intervals [see Dosage and Administration (2.4)].

Hypersensitivity reactions, including rash, urticaria, and fatal anaphylaxis, have occurred with other interleukin-6 receptor antagonists.

Because clinical studies are conducted under widely varying conditions, adverse reaction rates observed in the clinical studies of a drug cannot be directly compared to rates in the clinical studies of another drug and may not reflect the rates observed in clinical practice.

The safety of ENSPRYNG was evaluated in two randomized, placebo-controlled clinical trials [Study 1 evaluated ENSPRYNG without concurrent immunosuppressive therapy (IST) and Study 2 evaluated ENSPRYNG with concurrent IST], which included 41 anti-AQP4 seropositive patients treated with ENSPRYNG in Study 1 and 26 anti-AQP4 seropositive patients treated with ENSPRYNG in Study 2 [see Clinical Studies (14)]. In the double-blind, controlled period, the median exposure time on ENSPRYNG treatment was approximately 2 years in Study 1 and approximately 3 years in Study 2. The median exposure time on placebo treatment was approximately 1 year in both Study 1 and Study 2.

Adverse reactions that occurred in Study 1 and Study 2 in more than 5% of patients treated with ENSPRYNG, and at a greater incidence than in patients who received placebo, are shown in Table 3 and Table 4, respectively. The most common adverse reactions (15% or greater with ENSPRYNG in either) were nasopharyngitis, headache, upper respiratory tract infection, gastritis, rash, arthralgia, extremity pain, fatigue, and nausea.

<div class="scrollingtable"><table width="75%"> <caption> <span>Table 3 Adverse Reactions Occurring in 4 or More Patients Treated with ENSPRYNG and Greater Incidence than Placebo in Study 1</span> </caption> <col align="left" valign="middle" width="50%"/> <col align="center" valign="middle" width="25%"/> <col align="center" valign="middle" width="25%"/> <thead> <tr class="First Last"> <th align="center" class="Lrule Rrule">Adverse Reaction</th><th align="center" class="Rrule">ENSPRYNG<br/>(N = 41)<br/>%</th><th align="center" class="Rrule">PLACEBO<br/>(N = 23)<br/>%</th> </tr> </thead> <tbody> <tr class="Botrule First"> <td align="left" class="Lrule Rrule">Rash</td><td align="center" class="Rrule">17</td><td align="center" class="Rrule">0</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Arthralgia</td><td align="center" class="Rrule">17</td><td align="center" class="Rrule">0</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Pain in extremity</td><td align="center" class="Rrule">15</td><td align="center" class="Rrule">9</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Fatigue</td><td align="center" class="Rrule">15</td><td align="center" class="Rrule">4</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Nausea</td><td align="center" class="Rrule">15</td><td align="center" class="Rrule">9</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Nasopharyngitis</td><td align="center" class="Rrule">12</td><td align="center" class="Rrule">4</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Pruritus</td><td align="center" class="Rrule">10</td><td align="center" class="Rrule">0</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Depression</td><td align="center" class="Rrule">10</td><td align="center" class="Rrule">0</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Cellulitis</td><td align="center" class="Rrule">10</td><td align="center" class="Rrule">0</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Neutropenia</td><td align="center" class="Rrule">10</td><td align="center" class="Rrule">4</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Blood creatine phosphokinase increased</td><td align="center" class="Rrule">10</td><td align="center" class="Rrule">4</td> </tr> <tr class="Last"> <td align="left" class="Lrule Rrule">Fall</td><td align="center" class="Rrule">10</td><td align="center" class="Rrule">4</td> </tr> </tbody> </table></div>

<div class="scrollingtable"><table width="75%"> <caption> <span>Table 4 Adverse Reactions Occurring in 3 or More Patients Treated with ENSPRYNG and Greater Incidence than Placebo in Study 2</span> </caption> <col align="left" valign="middle" width="50%"/> <col align="center" valign="middle" width="25%"/> <col align="center" valign="middle" width="25%"/> <thead> <tr class="First Last"> <th align="center" class="Lrule Rrule">Adverse Reaction</th><th align="center" class="Rrule">ENSPRYNG + IST<br/>(N = 26)<br/>%</th><th align="center" class="Rrule">PLACEBO + IST<br/>(N = 26)<br/>%</th> </tr> </thead> <tbody> <tr class="Botrule First"> <td align="left" class="Lrule Rrule">Nasopharyngitis</td><td align="center" class="Rrule">31</td><td align="center" class="Rrule">15</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Headache</td><td align="center" class="Rrule">27</td><td align="center" class="Rrule">12</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Upper respiratory tract infection</td><td align="center" class="Rrule">19</td><td align="center" class="Rrule">12</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Gastritis</td><td align="center" class="Rrule">15</td><td align="center" class="Rrule">0</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule">Arthralgia</td><td align="center" class="Rrule">12</td><td align="center" class="Rrule">0</td> </tr> <tr class="Last"> <td align="left" class="Lrule Rrule">Pharyngitis</td><td align="center" class="Rrule">12</td><td align="center" class="Rrule">8</td> </tr> </tbody> </table></div>

Injection-Related Reactions

In Study 1 and Study 2, injection-related reactions were reported in 9% of patients treated with ENSPRYNG compared with 8% in patients receiving placebo. These reactions in the ENSPRYNG-treated patients were predominantly mild to moderate in severity, and most occurred within 24 hours after the injection. The most commonly reported systemic symptom was diarrhea. The reported local injection site reactions were pruritus, injection site reaction, and skin mass.

Infections

In Study 1, the rate of patients with infections was 51 patients/100 patient-years (95% CI: 32, 78) in patients treated with ENSPRYNG compared with 108 patients/100 patient-years (95% CI: 52, 199) in patients receiving placebo. The rate of patients with serious infections was 5 patients/100 patient-years (95% CI: 1, 14) in patients treated with ENSPRYNG compared with 4 patients/100 patient-years (95% CI: 0, 21) in patients receiving placebo.

In Study 2, the rate of patients with infections was 168 patients/100 patient-years (95% CI: 100, 265) in patients treated with ENSPRYNG compared with 143 patients/100 patient-years (95% CI: 83, 229) in patients treated with placebo. The rate of patients with serious infections was 4 patients/100 patient-years (95% CI: 1, 15) in patients treated with ENSPRYNG compared with 10 patients/100 patient-years (95% CI: 2, 28) in patients receiving placebo.

Laboratory Abnormalities

Decreased Neutrophil Count

Of the patients treated with ENSPRYNG, 10% had neutrophils below 1 × 109/L compared to 9% in placebo in Study 1. In Study 2, 15% patients had neutrophils below 1 × 109/L compared to 4% in placebo. There was one patient in Study 1 treated with ENSPRYNG with neutrophil counts < 0.5 × 109/L, and one patient in Study 2 discontinued ENSPRYNG because of neutropenia.

Decreased Platelet Count

In Study 1, a shift in platelet count decreases from normal at baseline to below the lower limit of normal (LLN) occurred in 26% of patients treated with ENSPRYNG compared to 5% of patients receiving placebo. In Study 2, decreases in platelet counts from normal at baseline to below the LLN occurred in 35% of patients treated with ENSPRYNG and in 17% of patients receiving placebo. None of the patients had a decrease in platelet count to less than 50 × 109/L.

Elevated Liver Enzymes

In Study 1, increases from normal at baseline to above ULN in ALT or AST occurred in 43% and 25% of patients treated with ENSPRYNG, respectively, compared to 13% and 9% of patients receiving placebo. In Study 2, increases from normal at baseline to above the ULN in ALT or AST occurred in 8% and 8% of patients treated with ENSPRYNG, respectively, compared to 12% and 19% of patients receiving placebo.

In Study 1 and Study 2 combined, elevations of ALT or AST greater than 3 times the ULN occurred in 3% of patients treated with ENSPRYNG, compared to no patients treated with placebo. These elevations were not associated with increases in total bilirubin. One patient receiving ENSPRYNG in Study 2 had an elevation of ALT above 5 times the ULN, which was observed 4 weeks after initiation of therapy, normalizing 78 days after discontinuation of ENSPRYNG.

Lipid Abnormalities

In Study 1 and Study 2, elevations in total cholesterol above 7.75 mmol/L (300 mg/dl) occurred in 12% and 15% of patients treated with ENSPRYNG, respectively, compared to no patients receiving placebo.

Elevations in triglycerides above 3.42 mmol/L (300 mg/dl) occurred in 27% and 12% of patients treated with ENSPRYNG in Study 1 and Study 2, respectively, compared to 13% and 8% of patients receiving placebo.

Fibrinogen Levels

In Study 1, the median percent reduction in fibrinogen was 38% in patients treated with ENSPRYNG compared to 5% in patients receiving placebo. In Study 2, the median percent reduction in fibrinogen level was 33% in patients treated with ENSPRYNG compared to 0% in patients receiving placebo.

Complement Levels

In Study 1, the median percent reduction in the C3 and C4 components of complement was 23% and 50% in patients treated with ENSPRYNG, respectively, compared to 0% and 1% patients receiving placebo. In Study 2, the median percent reduction in the C3 and C4 components of complement was 20% and 53% in patients treated with ENSPRYNG, respectively, compared to 0% and 1% in patients receiving placebo.

Body Weight

In the pool of Studies 1 and 2, body weight increases of at least 7% from baseline occurred in 28% of patients treated with ENSPRYNG compared to 8% of patients receiving placebo.

Body weight increases of at least 15% from baseline occurred in 4% of patients treated with ENSPRYNG compared to 4% of patients receiving placebo.

As with all therapeutic proteins, there is a potential for immunogenicity. The detection of antibody formation is highly dependent on the sensitivity and specificity of the assay. Additionally, the observed incidence of antibody (including neutralizing antibody) positivity in an assay may be influenced by several factors, including assay methodology, sample handling, timing of sample collection, concomitant medications, and underlying disease. For these reasons, comparison of the incidence of anti-satralizumab-mwge antibodies in the studies described below with the incidence of antibodies in other studies or to other products may be misleading.

In Study 1 and Study 2, anti-drug-antibodies (ADAs) were observed in 73% and 38% of patients receiving ENSPRYNG in the double-blind period, respectively. The ability of these ADAs to neutralize satralizumab-mwge binding is unknown. Patients with higher body weight and lower exposure were more likely to develop ADAs (irrespective of treatment with IST). Exposure was lower in ADA positive patients. Although anti-satralizumab-mwge antibody development was not found to affect the efficacy of ENSPRYNG in these patients, the available data are too limited to make definitive conclusions. Immunogenicity does not have a clinically-relevant impact on safety. Based on the available information, neither dose interruption nor modification is warranted in those patients who develop ADAs.

Pregnancy Exposure Registry

There is a pregnancy exposure registry that monitors pregnancy outcomes in women exposed to ENSPRYNG during pregnancy. Healthcare providers are encouraged to register patients and pregnant women are encouraged to register themselves by calling 1-833-277-9338.

Risk Summary

There are no adequate data on the developmental risk associated with the use of ENSPRYNG in pregnant women. In an animal reproduction study, no adverse effects on maternal animals or fetal development were observed in pregnant monkeys and their offspring, with administration of satralizumab-mwge at doses up to 50 mg/kg/week (see Data).

In the U.S. general population, the estimated background risk of major birth defect and miscarriage in clinically recognized pregnancies is 2 – 4% and 15 – 20%, respectively. The estimated background risk of major birth defects and miscarriage for the indicated population is unknown.

Clinical Considerations

Fetal/neonatal adverse reactions

Monoclonal antibodies are increasingly transported across the placenta as pregnancy progresses, with the largest amount transferred during the third trimester. Risks and benefits should be considered prior to administering live or live-attenuated vaccines to infants exposed to ENSPRYNG in utero [see Warnings and Precautions (5.1)].

Data

Animal Data

Weekly subcutaneous administration of satralizumab-mwge (0, 2, or 50 mg/kg) to monkeys throughout pregnancy resulted in no adverse effects on postnatal development of the offspring; however, immune function was impaired in offspring at both doses. Plasma exposures (Cave) in dams at the low and high doses were approximately 3 and 100 times, respectively, that in humans at the recommended monthly maintenance dose of 120 mg.

Risk Summary

No information is available on the presence of satralizumab-mwge in human milk, the effects of the satralizumab-mwge on the breastfed infant, or the effects of the satralizumab-mwge on milk production. Satralizumab-mwge was excreted in the milk of lactating monkeys administered satralizumab-mwge throughout pregnancy. Human IgG is excreted in human milk and the potential for absorption in the infant is unknown. The developmental and health benefits of breastfeeding should be considered along with the mother's clinical need for ENSPRYNG and any potential adverse effects on the breastfed infant from ENSPRYNG or from the underlying maternal condition.

Safety and effectiveness in pediatric patients have not been established.

Clinical studies of ENSPRYNG did not include sufficient numbers of patients aged 65 years and older to determine whether they respond differently from younger patients. However, population pharmacokinetic analyses in patients with NMOSD did not show that age affected the pharmacokinetics of satralizumab-mwge [see Clinical Pharmacology (12.3)]. In general, caution should be used when dosing the elderly, reflecting the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant diseases or other drug therapy.

Satralizumab-mwge is a recombinant humanized anti-human interleukin 6 (IL-6) receptor monoclonal antibody based on a human IgG2 framework. Each light chain and heavy chain consists of 214 and 443 amino acids, respectively. Satralizumab-mwge is a glycoprotein with an approximate molecular weight of 143 kDa and is produced by recombinant DNA technology in Chinese hamster ovary cells. The binding of satralizumab-mwge to the IL-6 receptor is pH-sensitive.

{ "type": "p", "children": [], "text": "Satralizumab-mwge is a recombinant humanized anti-human interleukin 6 (IL-6) receptor monoclonal antibody based on a human IgG2 framework. Each light chain and heavy chain consists of 214 and 443 amino acids, respectively. Satralizumab-mwge is a glycoprotein with an approximate molecular weight of 143 kDa and is produced by recombinant DNA technology in Chinese hamster ovary cells. The binding of satralizumab-mwge to the IL-6 receptor is pH-sensitive." }

ENSPRYNG (satralizumab-mwge) injection for subcutaneous administration is supplied as a sterile, clear, colorless to slightly yellow solution with no preservative with an approximate pH of 6. ENSPRYNG is supplied in a single-dose prefilled syringe. Each syringe delivers 1 mL of solution containing 120 mg of satralizumab-mwge, L-arginine (26.1 mg), L-histidine (3.1 mg), poloxamer 188 (0.5 mg), L-aspartic acid (pH adjustment), and Water for Injection, USP.

{ "type": "p", "children": [], "text": "ENSPRYNG (satralizumab-mwge) injection for subcutaneous administration is supplied as a sterile, clear, colorless to slightly yellow solution with no preservative with an approximate pH of 6. ENSPRYNG is supplied in a single-dose prefilled syringe. Each syringe delivers 1 mL of solution containing 120 mg of satralizumab-mwge, L-arginine (26.1 mg), L-histidine (3.1 mg), poloxamer 188 (0.5 mg), L-aspartic acid (pH adjustment), and Water for Injection, USP." }

The precise mechanism by which satralizumab-mwge exerts therapeutic effects in NMOSD is unknown but is presumed to involve inhibition of IL-6-mediated signaling through binding to soluble and membrane-bound IL-6 receptors.

The relationship between any of the pharmacodynamic effects of ENSPRYNG and clinical outcomes in NMOSD is unknown.

The pharmacokinetics of ENSPRYNG have been characterized both in Japanese and Caucasian healthy volunteers, and in NMOSD patients. The pharmacokinetics in NMOSD patients using the recommended dose were characterized using population pharmacokinetic analysis methods based on a database of 154 patients.

The concentration-time course of ENSPRYNG in patients with NMOSD was accurately described by a two-compartment population pharmacokinetic model with parallel linear and target-mediated (Michaelis-Menten) elimination and first-order subcutaneous absorption. ENSPRYNG clearance and volume parameters allometrically scaled by body weight (through power function with the fixed power coefficient of 0.75 and 1 for clearance and volume parameters, respectively). Body weight was shown to be a significant covariate, with clearance and Vc for patients weighing 123 kg (97.5th percentile of the weight distribution) increased by 71.3% and 105%, respectively, compared to a patient weighing 60 kg.

Steady state pharmacokinetics were achieved after the loading period (8 weeks) as follows [mean (±SD)]: Cmin: 19.7 (12.2) mcg/mL, Cmax: 31.5 (14.9) mcg/mL, and AUC: 737 (386) mcg.mL/day.

Absorption

The bioavailability of satralizumab-mwge was 85%.

Distribution

Satralizumab-mwge undergoes biphasic distribution. The central volume of distribution was 3.46 L and the peripheral volume of distribution was 2.07 L. The inter-compartmental clearance was 0.336 L/day.

Elimination

The total clearance of satralizumab-mwge is concentration-dependent. Linear clearance (accounting for approximately half of the total clearance at steady state using the recommended dose in NMOSD patients) is estimated to be 0.0601 L/day. The associated terminal t1/2 is approximately 30 days (range 22 – 37 days) based on data pooled from Study 1 and Study 2.

Metabolism

The metabolism of satralizumab-mwge has not been directly studied, as antibodies are cleared principally by catabolism.

Excretion

Monoclonal antibodies, including satralizumab-mwge, are not eliminated via renal or hepatic pathways.

Specific Populations

Population pharmacokinetic analyses in patients with NMOSD showed that age, gender, and race did not meaningfully influence the pharmacokinetics of satralizumab-mwge.

Patients with Renal or Hepatic Impairment

No formal studies of the effect of renal impairment or hepatic impairment on the pharmacokinetics of satralizumab-mwge were conducted.

Drug Interaction Studies

No formal drug-drug interaction studies have been performed with ENSPRYNG.

Based on population pharmacokinetic analyses of the available data, the impact of commonly used small molecule drugs on the pharmacokinetics of satralizumab-mwge remains inconclusive.

Suppression of IL-6 signaling by treatment with ENSPRYNG, from the low baseline levels seen in Study 1 and Study 2, is expected to have a minor impact on exposure of concomitant medications metabolized by CYP450 enzymes. The clinical significance of this is unknown.

Carcinogenesis

Carcinogenicity studies of satralizumab-mwge were not conducted.

Mutagenesis

Genetic toxicology studies of satralizumab-mwge were not conducted. As an antibody, satralizumab-mwge is not expected to interact directly with DNA.

Impairment of Fertility

In monkeys administered satralizumab-mwge (0, 2, 10, or 50 mg/kg) weekly by subcutaneous injection for 26 weeks, no effects on sperm, estrus cycle, or male and female reproductive organs were observed. At the high dose, plasma exposures (Cave) were approximately 100 times that in humans at the recommended monthly maintenance dose of 120 mg.

The efficacy of ENSPRYNG for the treatment of NMOSD in adult patients was established in two studies. Study 1 was a randomized (2:1), placebo-controlled trial in 95 patients without concurrent IST (Study 1, NCT02073279) in which 64 patients were anti-AQP4 antibody positive and 31 patients were anti-AQP4 antibody negative.

{ "type": "p", "children": [], "text": "The efficacy of ENSPRYNG for the treatment of NMOSD in adult patients was established in two studies. Study 1 was a randomized (2:1), placebo-controlled trial in 95 patients without concurrent IST (Study 1, NCT02073279) in which 64 patients were anti-AQP4 antibody positive and 31 patients were anti-AQP4 antibody negative." }

Study 2 was a randomized (1:1), placebo-controlled trial in 76 adult patients with concurrent IST (Study 2, NCT02028884). Of these, 52 adult patients were anti-AQP4 antibody positive and 24 adult patients were anti-AQP4 antibody negative.

{ "type": "p", "children": [], "text": "Study 2 was a randomized (1:1), placebo-controlled trial in 76 adult patients with concurrent IST (Study 2, NCT02028884). Of these, 52 adult patients were anti-AQP4 antibody positive and 24 adult patients were anti-AQP4 antibody negative." }

Patients met the following eligibility criteria:

{ "type": "p", "children": [], "text": "Patients met the following eligibility criteria:" }

{ "type": "", "children": [], "text": "" }

In Study 1, 41 anti-AQP4 antibody positive adult patients were randomized to and received ENSPRYNG and 23 received placebo. Females accounted for 76% of the ENSPRYNG group and 96% of the placebo group. The remaining baseline demographic characteristics were balanced between the treatment groups. The mean age was 44 years. Fifty percent were White, 22% were Black or African-American, and 20% were Asian. The mean EDSS score was 3.8.

{ "type": "p", "children": [], "text": "In Study 1, 41 anti-AQP4 antibody positive adult patients were randomized to and received ENSPRYNG and 23 received placebo. Females accounted for 76% of the ENSPRYNG group and 96% of the placebo group. The remaining baseline demographic characteristics were balanced between the treatment groups. The mean age was 44 years. Fifty percent were White, 22% were Black or African-American, and 20% were Asian. The mean EDSS score was 3.8." }

In Study 2, 26 anti-AQP4 antibody positive adult patients were randomized to and received ENSPRYNG and 26 received placebo. All patients were receiving either concurrent azathioprine (42%), oral corticosteroids (52%), or mycophenolate mofetil (6%) during the trial. The baseline demographic and disease characteristics were balanced between the treatment groups. Females accounted for 100% of the study population. Forty-six percent of patients were White and 52% were Asian. The mean age was 46 years. The mean EDSS score was 4.0.

{ "type": "p", "children": [], "text": "In Study 2, 26 anti-AQP4 antibody positive adult patients were randomized to and received ENSPRYNG and 26 received placebo. All patients were receiving either concurrent azathioprine (42%), oral corticosteroids (52%), or mycophenolate mofetil (6%) during the trial. The baseline demographic and disease characteristics were balanced between the treatment groups. Females accounted for 100% of the study population. Forty-six percent of patients were White and 52% were Asian. The mean age was 46 years. The mean EDSS score was 4.0." }

All potential relapses were adjudicated by a blinded Clinical Endpoint Committee (CEC). The primary efficacy endpoint for both studies was the time to the first CEC-confirmed relapse.

{ "type": "p", "children": [], "text": "All potential relapses were adjudicated by a blinded Clinical Endpoint Committee (CEC). The primary efficacy endpoint for both studies was the time to the first CEC-confirmed relapse." }

In Study 1, the time to the first CEC-confirmed relapse was significantly longer in ENSPRYNG-treated patients compared to patients who received placebo (risk reduction 55%; hazard ratio 0.45; p = 0.0184). In the anti-AQP4 antibody positive population, there was a 74% risk reduction; hazard ratio 0.26; p = 0.0014 (Table 5; Figure 1). There was no evidence of a benefit in the anti-AQP4 antibody negative patients.

{ "type": "p", "children": [], "text": "In Study 1, the time to the first CEC-confirmed relapse was significantly longer in ENSPRYNG-treated patients compared to patients who received placebo (risk reduction 55%; hazard ratio 0.45; p = 0.0184). In the anti-AQP4 antibody positive population, there was a 74% risk reduction; hazard ratio 0.26; p = 0.0014 (Table 5; Figure 1). There was no evidence of a benefit in the anti-AQP4 antibody negative patients." }

In Study 2, the time to the first CEC-confirmed relapse was significantly longer in patients treated with ENSPRYNG compared to patients who received placebo (risk reduction 62%; hazard ratio 0.38; p = 0.0184). In the anti-AQP4 antibody positive population, there was a 78% risk reduction; hazard ratio 0.22; p = 0.0143 (Table 5; Figure 2). There was no evidence of a benefit in the anti-AQP4 antibody negative patients.

{ "type": "p", "children": [], "text": "In Study 2, the time to the first CEC-confirmed relapse was significantly longer in patients treated with ENSPRYNG compared to patients who received placebo (risk reduction 62%; hazard ratio 0.38; p = 0.0184). In the anti-AQP4 antibody positive population, there was a 78% risk reduction; hazard ratio 0.22; p = 0.0143 (Table 5; Figure 2). There was no evidence of a benefit in the anti-AQP4 antibody negative patients." }

<div class="scrollingtable"><table width="85%"> <caption> <span>Table 5 Efficacy Results from Study 1 and Study 2 in anti-AQP4 Antibody Positive NMOSD Patients</span> </caption> <col align="center" valign="top" width="36%"/> <col align="center" valign="top" width="16%"/> <col align="center" valign="top" width="16%"/> <col align="center" valign="top" width="16%"/> <col align="center" valign="top" width="16%"/> <thead> <tr class="Botrule First"> <th align="center" class="Lrule Rrule"></th><th align="center" class="Rrule" colspan="2">Study 1</th><th align="center" class="Rrule" colspan="2">Study 2</th> </tr> <tr class="Botrule"> <th align="center" class="Lrule Rrule"></th><th align="center" class="Rrule">ENSPRYNG<br/>N=41</th><th align="center" class="Rrule">Placebo<br/>N=23</th><th align="center" class="Rrule">ENSPRYNG + IST<a class="Sup" href="#footnote-3" name="footnote-reference-3">*</a> <br/>N= 26</th><th align="center" class="Rrule">Placebo + IST<br/>N=26</th> </tr> <tr class="Last"> <th align="center" class="Lrule Rrule" colspan="5">Time to Clinical Endpoint Committee (CEC)-Determined Relapse (Primary Efficacy Endpoint)</th> </tr> </thead> <tfoot> <tr> <td align="left" colspan="5"> <dl class="Footnote"> <dt> <a href="#footnote-reference-3" name="footnote-3">*</a> </dt> <dd>IST = immunosuppressant therapy</dd> </dl> </td> </tr> </tfoot> <tbody> <tr class="Botrule First"> <td align="center" class="Lrule Rrule"><span class="Bold">Number (%) of Patients with Relapse</span></td><td align="center" class="Rrule">9 (22)</td><td align="center" class="Rrule">13 (56.5)</td><td align="center" class="Rrule">3 (11.5)</td><td align="center" class="Rrule">11 (42.3)</td> </tr> <tr class="Botrule"> <td align="center" class="Lrule Rrule"><span class="Bold">Hazard Ratio (95% CI)</span></td><td align="center" class="Rrule" colspan="2">0.26<br/>(0.11, 0.63)</td><td align="center" class="Rrule" colspan="2">0.22<br/>(0.06, 0.82)</td> </tr> <tr class="Botrule"> <td align="center" class="Lrule Rrule"><span class="Bold">p-value</span></td><td align="center" class="Rrule" colspan="2">0.0014</td><td align="center" class="Rrule" colspan="2">0.0143</td> </tr> <tr class="Botrule"> <td align="center" class="Lrule Rrule"><span class="Bold">Risk Reduction</span></td><td align="center" class="Rrule" colspan="2">74%</td><td align="center" class="Rrule" colspan="2">78%</td> </tr> <tr class="Last"> <td align="center" class="Lrule Rrule"><span class="Bold">Proportion of Protocol Defined Relapse-Free Patients at 96 Weeks</span></td><td align="center" class="Rrule">76.5%</td><td align="center" class="Rrule">41.1%</td><td align="center" class="Rrule">91.1%</td><td align="center" class="Rrule">56.8%</td> </tr> </tbody> </table></div>

{ "type": "table", "children": [], "text": "<div class=\"scrollingtable\"><table width=\"85%\">\n<caption>\n<span>Table 5 Efficacy Results from Study 1 and Study 2 in anti-AQP4 Antibody Positive NMOSD Patients</span>\n</caption>\n<col align=\"center\" valign=\"top\" width=\"36%\"/>\n<col align=\"center\" valign=\"top\" width=\"16%\"/>\n<col align=\"center\" valign=\"top\" width=\"16%\"/>\n<col align=\"center\" valign=\"top\" width=\"16%\"/>\n<col align=\"center\" valign=\"top\" width=\"16%\"/>\n<thead>\n<tr class=\"Botrule First\">\n<th align=\"center\" class=\"Lrule Rrule\"></th><th align=\"center\" class=\"Rrule\" colspan=\"2\">Study 1</th><th align=\"center\" class=\"Rrule\" colspan=\"2\">Study 2</th>\n</tr>\n<tr class=\"Botrule\">\n<th align=\"center\" class=\"Lrule Rrule\"></th><th align=\"center\" class=\"Rrule\">ENSPRYNG<br/>N=41</th><th align=\"center\" class=\"Rrule\">Placebo<br/>N=23</th><th align=\"center\" class=\"Rrule\">ENSPRYNG + IST<a class=\"Sup\" href=\"#footnote-3\" name=\"footnote-reference-3\">*</a>\n<br/>N= 26</th><th align=\"center\" class=\"Rrule\">Placebo + IST<br/>N=26</th>\n</tr>\n<tr class=\"Last\">\n<th align=\"center\" class=\"Lrule Rrule\" colspan=\"5\">Time to Clinical Endpoint Committee (CEC)-Determined Relapse (Primary Efficacy Endpoint)</th>\n</tr>\n</thead>\n<tfoot>\n<tr>\n<td align=\"left\" colspan=\"5\">\n<dl class=\"Footnote\">\n<dt>\n<a href=\"#footnote-reference-3\" name=\"footnote-3\">*</a>\n</dt>\n<dd>IST = immunosuppressant therapy</dd>\n</dl>\n</td>\n</tr>\n</tfoot>\n<tbody>\n<tr class=\"Botrule First\">\n<td align=\"center\" class=\"Lrule Rrule\"><span class=\"Bold\">Number (%) of Patients with Relapse</span></td><td align=\"center\" class=\"Rrule\">9 (22)</td><td align=\"center\" class=\"Rrule\">13 (56.5)</td><td align=\"center\" class=\"Rrule\">3 (11.5)</td><td align=\"center\" class=\"Rrule\">11 (42.3)</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"center\" class=\"Lrule Rrule\"><span class=\"Bold\">Hazard Ratio (95% CI)</span></td><td align=\"center\" class=\"Rrule\" colspan=\"2\">0.26<br/>(0.11, 0.63)</td><td align=\"center\" class=\"Rrule\" colspan=\"2\">0.22<br/>(0.06, 0.82)</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"center\" class=\"Lrule Rrule\"><span class=\"Bold\">p-value</span></td><td align=\"center\" class=\"Rrule\" colspan=\"2\">0.0014</td><td align=\"center\" class=\"Rrule\" colspan=\"2\">0.0143</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"center\" class=\"Lrule Rrule\"><span class=\"Bold\">Risk Reduction</span></td><td align=\"center\" class=\"Rrule\" colspan=\"2\">74%</td><td align=\"center\" class=\"Rrule\" colspan=\"2\">78%</td>\n</tr>\n<tr class=\"Last\">\n<td align=\"center\" class=\"Lrule Rrule\"><span class=\"Bold\">Proportion of Protocol Defined Relapse-Free Patients at 96 Weeks</span></td><td align=\"center\" class=\"Rrule\">76.5%</td><td align=\"center\" class=\"Rrule\">41.1%</td><td align=\"center\" class=\"Rrule\">91.1%</td><td align=\"center\" class=\"Rrule\">56.8%</td>\n</tr>\n</tbody>\n</table></div>" }

Figure 1 Study 1: Time to First CEC-Determined NMOSD Relapse in the Randomized Controlled Period in the ITT Population Anti-AQP4 Antibody Positive Patients

{ "type": "p", "children": [], "text": "\nFigure 1 Study 1: Time to First CEC-Determined NMOSD Relapse in the Randomized Controlled Period in the ITT Population Anti-AQP4 Antibody Positive Patients\n" }

Figure 2 Study 2: Time to First CEC-Determined NMOSD Relapse in the Randomized Controlled Period in the ITT Population Anti-AQP4 Antibody Positive Patients

{ "type": "p", "children": [], "text": "\nFigure 2 Study 2: Time to First CEC-Determined NMOSD Relapse in the Randomized Controlled Period in the ITT Population Anti-AQP4 Antibody Positive Patients\n" }

ENSPRYNG (satralizumab-mwge) injection is available as a sterile, preservative-free, clear, colorless to slightly yellow solution in single-dose prefilled syringe (PFS) with needle safety device.

ENSPRYNG PFS is not made with natural rubber latex. Each ENSPRYNG carton contains one single-dose 120 mg/mL prefilled syringe (NDC 50242-007-01).

Infections

Inform patients that an increased risk of infections, including serious and potentially fatal infections, has been observed in patients treated with IL-6 receptor antagonists, including ENSPRYNG. Instruct patients to contact their healthcare provider immediately when symptoms suggesting infection (e.g., fever, chills, constant cough, or sore throat) appear during treatment [see Warning and Precautions (5.1)].

Vaccinations

Advise patients to complete any required vaccinations at least 4 weeks prior to initiation of ENSPRYNG for live or live-attenuated vaccines and, whenever possible, at least 2 weeks prior to initiation of ENSPRYNG for non-live vaccines [see Warnings and Precautions 5.1].

Elevated Liver Enzymes

Inform patients on the importance of liver enzyme testing [see Warnings and Precautions (5.2)].

Decreased Neutrophil Counts

Inform patients on the importance of neutrophil count testing [see Warnings and Precautions (5.3)].

Hypersensitivity Reactions

Inform patients about the signs and symptoms of hypersensitivity reactions and anaphylaxis and advise them to contact their healthcare provider immediately if these symptoms occur [see Warnings and Precautions (5.4)].

Instruction on Injection Technique

Instruct patients and caregivers to read the Instructions for Use before the patient starts using ENSPRYNG, and each time the patient gets a refill as there may be new information they need to know.

Perform the first injection under the guidance of a qualified healthcare professional. If a patient or caregiver is to administer subcutaneous ENSPRYNG, instruct him/her in injection techniques and assess his/her ability to inject subcutaneously to ensure proper administration of subcutaneous ENSPRYNG and the suitability for home use [see Dosage and Administration (2.3) and Instructions for Use].

Instruct patients to remove the prefilled syringe from the refrigerator prior to use and allow to sit at room temperature outside of the carton for 30 minutes. Do not warm ENSPRYNG in any other way.

Advise patients to consult their healthcare provider if the full dose is not received.

A puncture-resistant container for disposal of syringes should be used and should be kept out of the reach of children. Instruct patients or caregivers in the technique as well as proper prefilled syringe disposal, and caution against reuse of these items.

Pregnancy Exposure Registry

Encourage patients to enroll in the ENSPRYNG Pregnancy Registry if they become pregnant while taking ENSPRYNG. The Registry monitors fetal outcomes of pregnant women exposed to ENSPRYNG [see Use in Specific Populations (8.1)].

ENSPRYNG® [satralizumab-mwge]

{ "type": "p", "children": [], "text": "ENSPRYNG® [satralizumab-mwge]" }

Manufactured by: Genentech, Inc. A Member of the Roche Group1 DNA WaySouth San Francisco, CA 94080-4990

{ "type": "p", "children": [], "text": "Manufactured by:\nGenentech, Inc. \t\t\t\t\t\t\tA Member of the Roche Group1 DNA WaySouth San Francisco, CA 94080-4990" }

ENSPRYNG® is a registered trademark ofChugai Pharmaceutical Co., Ltd., Tokyo, Japan©2022 Genentech, Inc. All rights reserved.

{ "type": "p", "children": [], "text": "ENSPRYNG® is a registered trademark ofChugai Pharmaceutical Co., Ltd., Tokyo, Japan©2022 Genentech, Inc. All rights reserved." }

U.S. License No.: 1048

{ "type": "p", "children": [], "text": "U.S. License No.: 1048" }

<div class="scrollingtable"><table width="100%"> <col align="left" valign="top" width="4%"/> <col align="left" valign="top" width="47%"/> <col align="left" valign="top" width="49%"/> <tfoot> <tr class="First Last"> <td align="left" colspan="2" valign="top">This <a href="#MG">Medication Guide</a> has been approved by the U.S. Food and Drug Administration</td><td align="right" valign="top">Issued: 3/2022</td> </tr> </tfoot> <tbody class="Headless"> <tr class="Botrule First"> <td align="center" class="Lrule Rrule" colspan="3"><span class="Bold">MEDICATION GUIDE</span> <br/>ENSPRYNG<span class="Sup">®</span> (en-spryng)<br/>(satralizumab-mwge)<br/>injection, for subcutaneous use</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold"><a name="whatis"></a>What is the most important information I should know about ENSPRYNG?<br/>ENSPRYNG may cause serious side effects including:</span> <dl> <dt class="Bold">1.</dt> <dd> <span class="Bold">Infections.</span> ENSPRYNG can increase your risk of serious infections some of which can be life-threatening. Talk to your healthcare provider if you are being treated for an infection or call them right away if you think you have signs of an infection, with or without a fever, such as:<ul class="Circle"> <li>chills, feeling tired, muscle aches, cough that will not go away or a sore throat</li> <li>skin redness, swelling, tenderness, pain or sores on your body</li> <li>diarrhea, belly pain, or feeling sick</li> <li>burning when you urinate or urinating more often than usual</li> </ul>Your healthcare provider will check if you have an infection and treat it if needed before you start or continue to take ENSPRYNG. </dd> </dl> <ul> <li>Your healthcare provider should test you for hepatitis and tuberculosis (TB) before you start taking ENSPRYNG.</li> <li>All required vaccinations should be completed before starting ENSPRYNG. People using ENSPRYNG should not be given 'live' or 'live-attenuated' vaccines. 'Live' or 'live-attenuated' vaccines should be given at least 4 weeks before you start ENSPRYNG. Your healthcare provider may recommend that you get a 'non-live' (inactivated) vaccine, such as some of the seasonal flu vaccines. If you plan to get a 'non-live' (inactivated) vaccine, it should be given, whenever possible, at least 2 weeks before you start ENSPRYNG.</li> </ul> <dl> <dt class="Bold">2.</dt> <dd> <span class="Bold">Increased liver enzymes.</span> <br/>Your healthcare provider should order blood tests to check your liver enzymes before and while you are taking ENSPRYNG. Your healthcare provider will tell you how often you will need to have these blood tests. Make sure you get all of your follow-up blood tests as ordered by your healthcare provider. Your healthcare provider will tell you if you need to wait to start ENSPRYNG if your liver enzymes are increased.</dd> <dt class="Bold">3.</dt> <dd> <span class="Bold">Low neutrophil count.</span> <br/>ENSPRYNG can cause a decrease in your neutrophil counts in your blood. Neutrophils are white blood cells that help the body fight off bacterial infections. Your healthcare provider should order blood tests to check your neutrophil count while you are taking ENSPRYNG.</dd> </dl> <span class="Bold">See "<a href="#whatare">What are the possible side effects with ENSPRYNG?</a>"</span></td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold">What is ENSPRYNG?</span> <br/>ENSPRYNG is a prescription medicine used to treat neuromyelitis optica spectrum disorder (NMOSD) in adults who are aquaporin-4 (AQP4) antibody positive.<br/>It is not known if ENSPRYNG is safe and effective in children.</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold">Do not take ENSPRYNG if you:</span> <ul> <li>are allergic to satralizumab-mwge or any of the ingredients in ENSPRYNG. See <span class="Bold">"<a href="#ingredients">What are the ingredients in ENSPRYNG?</a>"</span> at the end of this <a href="#MG">Medication Guide</a> for a complete list of ingredients in ENSPRYNG.</li> <li>have an active hepatitis B infection.</li> <li>have active or untreated inactive (latent) TB. </li> </ul> </td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold">Before you take ENSPRYNG, tell your healthcare provider about all of your medical conditions, including if you:</span> <ul> <li>have or think you have an infection. See <span class="Bold">"<a href="#whatis">What is the most important information I should know about ENSPRYNG?</a>"</span> </li> <li>have liver problems.</li> <li>have ever had hepatitis B or are a carrier of the hepatitis B virus.</li> <li>have had or have been in contact with someone with tuberculosis.</li> <li>have had a recent vaccination or are scheduled to receive any vaccination.</li> <li>are pregnant, think that you might be pregnant, or plan to become pregnant. It is not known if ENSPRYNG will harm your unborn baby.<ul class="Circle"> <li> <span class="Bold">Pregnancy Registry</span>: There is a registry for pregnant women who take ENSPRYNG. The purpose of this registry is to check the health of the pregnant mother and her baby. If you are pregnant or become pregnant while taking ENSPRYNG, talk to your healthcare provider about how you can join this pregnancy registry or you may contact the registry at 1-833-277-9338 to enroll.</li> </ul> </li> <li>are breastfeeding or plan to breastfeed. It is not known if ENSPRYNG passes into your breast milk. Talk to your healthcare provider about the best way to feed your baby if you take ENSPRYNG.</li> </ul> <span class="Bold">Tell your healthcare provider about all the medicines you are taking,</span> including prescription and over-the-counter medicines, vitamins, and herbal supplements. </td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold">How should I take ENSPRYNG?</span> <ul> <li>ENSPRYNG is provided as a solution in a single-dose, prefilled syringe of 120 mg/mL of satralizumab-mwge.</li> <li>See the <span class="Bold"><a href="#IFU">Instructions for Use</a></span> inside the carton for complete instructions for the right way to prepare and inject ENSPRYNG.</li> <li>ENSPRYNG is given by an injection under the skin (subcutaneously). If your healthcare provider decides that you or your caregiver can give your injections of ENSPRYNG, you or your caregiver should receive training on the right way to prepare and inject ENSPRYNG.</li> <li>Always inject all of the medicine in the syringe.</li> <li>The first 3 injections (loading period) of ENSPRYNG are taken 1 time every 2 weeks.</li> <li>After this, injection of ENSPRYNG is taken every 4 weeks (maintenance period). Keep taking ENSPRYNG 1 time every 4 weeks for as long as your healthcare provider tells you to.</li> <li>If you miss a dose of ENSPRYNG, talk to your health care provider about restarting dosing.</li> </ul> </td> </tr> <tr> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold"><a name="whatare"></a>What are the possible side effects of ENSPRYNG?<br/>ENSPRYNG may cause serious side effects, including:</span> <ul> <li>See <span class="Bold">"<a href="#whatis">What is the most important information I should know about ENSPRYNG?</a>"</span> </li> <li> <span class="Bold">Serious allergic reactions.</span> Serious allergic reactions that may be life-threatening have happened with other medicines like ENSPRYNG. Tell your healthcare provider before taking your next dose if you had hives, rash, or flushing after your injection. Seek medical attention right away if you have any symptoms of a serious allergic reaction, such as:</li> </ul> </td> </tr> <tr> <td align="left" class="Lrule"></td><td align="left"> <ul class="Circle"> <li>shortness of breath or trouble breathing </li> <li>dizziness or feeling faint</li> </ul> </td><td align="left" class="Rrule"> <ul class="Circle"> <li>swelling of your lips, face, or tongue</li> <li>moderate or severe stomach (abdominal) pain or vomiting</li> <li>chest pain</li> </ul> </td> </tr> <tr> <td align="left" class="Lrule Rrule" colspan="3"> <ul> <li>The most common side effects of ENSPRYNG include:</li> </ul> </td> </tr> <tr> <td align="left" class="Lrule"></td><td align="left"> <ul class="Circle"> <li>sore throat, runny nose (nasopharyngitis)</li> <li>rash</li> <li>fatigue</li> <li>extremity pain</li> </ul> </td><td align="left" class="Rrule"> <ul class="Circle"> <li>headache</li> <li>upper respiratory tract infection</li> <li>nausea</li> <li>inflammation of the stomach lining (gastritis)</li> <li>joint pain</li> </ul> </td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3">These are not all the possible side effects of ENSPRYNG.<br/>Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800-FDA-1088. You may also report side effects to Genentech at 1-888-835-2555.</td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold">How should I store ENSPRYNG?</span> <ul> <li>Store ENSPRYNG in the refrigerator between 36°F to 46°F (2°C to 8°C) in the original carton.</li> <li>Protect from light.</li> <li> <span class="Bold">Do not</span> freeze or use the syringe if it has been frozen.</li> <li> <span class="Bold">Do not</span> shake.</li> <li>ENSPRYNG, if unopened, can be removed from and returned to the refrigerator, if needed. The total combined time out of the refrigerator should not be more than 8 days at a temperature that does not go above 86°F (30°C).</li> </ul> </td> </tr> <tr class="Botrule"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold">General information about the safe and effective use of ENSPRYNG.</span> <br/>Medicines are sometimes prescribed for purposes other than those listed in a <a href="#MG">Medication Guide</a>. Do not use ENSPRYNG for a condition for which it was not prescribed. Do not give ENSPRYNG to other people, even if they have the same symptoms that you have. It may harm them. You can ask your pharmacist or healthcare provider for information about ENSPRYNG that is written for health professionals.</td> </tr> <tr class="Last"> <td align="left" class="Lrule Rrule" colspan="3"><span class="Bold"><a name="ingredients"></a>What are the ingredients in ENSPRYNG?</span> <br/> <span class="Bold">Active ingredient:</span> satralizumab-mwge<br/> <span class="Bold">Inactive ingredients:</span> L-arginine, L-histidine, poloxamer 188, L-aspartic acid, and Water for Injection.<br/>Manufactured by: <span class="Bold">Genentech, Inc.</span>, A Member of the Roche Group, 1 DNA Way, South San Francisco, CA 94080-4990<br/>ENSPRYNG<span class="Sup">®</span> is a registered trademark of Chugai Pharmaceutical Co., Ltd., Tokyo, Japan<br/>U.S. License No.: 1048<br/>For more information, go to www.ENSPRYNG.com or call 1-844-NSPRYNG.</td> </tr> </tbody> </table></div>

{ "type": "table", "children": [], "text": "<div class=\"scrollingtable\"><table width=\"100%\">\n<col align=\"left\" valign=\"top\" width=\"4%\"/>\n<col align=\"left\" valign=\"top\" width=\"47%\"/>\n<col align=\"left\" valign=\"top\" width=\"49%\"/>\n<tfoot>\n<tr class=\"First Last\">\n<td align=\"left\" colspan=\"2\" valign=\"top\">This <a href=\"#MG\">Medication Guide</a> has been approved by the U.S. Food and Drug Administration</td><td align=\"right\" valign=\"top\">Issued: 3/2022</td>\n</tr>\n</tfoot>\n<tbody class=\"Headless\">\n<tr class=\"Botrule First\">\n<td align=\"center\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">MEDICATION GUIDE</span>\n<br/>ENSPRYNG<span class=\"Sup\">®</span> (en-spryng)<br/>(satralizumab-mwge)<br/>injection, for subcutaneous use</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\"><a name=\"whatis\"></a>What is the most important information I should know about ENSPRYNG?<br/>ENSPRYNG may cause serious side effects including:</span>\n<dl>\n<dt class=\"Bold\">1.</dt>\n<dd>\n<span class=\"Bold\">Infections.</span> ENSPRYNG can increase your risk of serious infections some of which can be life-threatening. Talk to your healthcare provider if you are being treated for an infection or call them right away if you think you have signs of an infection, with or without a fever, such as:<ul class=\"Circle\">\n<li>chills, feeling tired, muscle aches, cough that will not go away or a sore throat</li>\n<li>skin redness, swelling, tenderness, pain or sores on your body</li>\n<li>diarrhea, belly pain, or feeling sick</li>\n<li>burning when you urinate or urinating more often than usual</li>\n</ul>Your healthcare provider will check if you have an infection and treat it if needed before you start or continue to take ENSPRYNG. \t\t\t\t\t\t\t\t\t\t\t</dd>\n</dl>\n<ul>\n<li>Your healthcare provider should test you for hepatitis and tuberculosis (TB) before you start taking ENSPRYNG.</li>\n<li>All required vaccinations should be completed before starting ENSPRYNG. People using ENSPRYNG should not be given 'live' or 'live-attenuated' vaccines. 'Live' or 'live-attenuated' vaccines should be given at least 4 weeks before you start ENSPRYNG. Your healthcare provider may recommend that you get a 'non-live' (inactivated) vaccine, such as some of the seasonal flu vaccines. If you plan to get a 'non-live' (inactivated) vaccine, it should be given, whenever possible, at least 2 weeks before you start ENSPRYNG.</li>\n</ul>\n<dl>\n<dt class=\"Bold\">2.</dt>\n<dd>\n<span class=\"Bold\">Increased liver enzymes.</span>\n<br/>Your healthcare provider should order blood tests to check your liver enzymes before and while you are taking ENSPRYNG. Your healthcare provider will tell you how often you will need to have these blood tests. Make sure you get all of your follow-up blood tests as ordered by your healthcare provider. Your healthcare provider will tell you if you need to wait to start ENSPRYNG if your liver enzymes are increased.</dd>\n<dt class=\"Bold\">3.</dt>\n<dd>\n<span class=\"Bold\">Low neutrophil count.</span>\n<br/>ENSPRYNG can cause a decrease in your neutrophil counts in your blood. Neutrophils are white blood cells that help the body fight off bacterial infections. Your healthcare provider should order blood tests to check your neutrophil count while you are taking ENSPRYNG.</dd>\n</dl>\n<span class=\"Bold\">See \"<a href=\"#whatare\">What are the possible side effects with ENSPRYNG?</a>\"</span></td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">What is ENSPRYNG?</span>\n<br/>ENSPRYNG is a prescription medicine used to treat neuromyelitis optica spectrum disorder (NMOSD) in adults who are aquaporin-4 (AQP4) antibody positive.<br/>It is not known if ENSPRYNG is safe and effective in children.</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">Do not take ENSPRYNG if you:</span>\n<ul>\n<li>are allergic to satralizumab-mwge or any of the ingredients in ENSPRYNG. See <span class=\"Bold\">\"<a href=\"#ingredients\">What are the ingredients in ENSPRYNG?</a>\"</span> at the end of this <a href=\"#MG\">Medication Guide</a> for a complete list of ingredients in ENSPRYNG.</li>\n<li>have an active hepatitis B infection.</li>\n<li>have active or untreated inactive (latent) TB. </li>\n</ul>\n</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">Before you take ENSPRYNG, tell your healthcare provider about all of your medical conditions, including if you:</span>\n<ul>\n<li>have or think you have an infection. See <span class=\"Bold\">\"<a href=\"#whatis\">What is the most important information I should know about ENSPRYNG?</a>\"</span>\n</li>\n<li>have liver problems.</li>\n<li>have ever had hepatitis B or are a carrier of the hepatitis B virus.</li>\n<li>have had or have been in contact with someone with tuberculosis.</li>\n<li>have had a recent vaccination or are scheduled to receive any vaccination.</li>\n<li>are pregnant, think that you might be pregnant, or plan to become pregnant. It is not known if ENSPRYNG will harm your unborn baby.<ul class=\"Circle\">\n<li>\n<span class=\"Bold\">Pregnancy Registry</span>: There is a registry for pregnant women who take ENSPRYNG. The purpose of this registry is to check the health of the pregnant mother and her baby. If you are pregnant or become pregnant while taking ENSPRYNG, talk to your healthcare provider about how you can join this pregnancy registry or you may contact the registry at 1-833-277-9338 to enroll.</li>\n</ul>\n</li>\n<li>are breastfeeding or plan to breastfeed. It is not known if ENSPRYNG passes into your breast milk. Talk to your healthcare provider about the best way to feed your baby if you take ENSPRYNG.</li>\n</ul>\n<span class=\"Bold\">Tell your healthcare provider about all the medicines you are taking,</span> including prescription and over-the-counter medicines, vitamins, and herbal supplements. </td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">How should I take ENSPRYNG?</span>\n<ul>\n<li>ENSPRYNG is provided as a solution in a single-dose, prefilled syringe of 120 mg/mL of satralizumab-mwge.</li>\n<li>See the <span class=\"Bold\"><a href=\"#IFU\">Instructions for Use</a></span> inside the carton for complete instructions for the right way to prepare and inject ENSPRYNG.</li>\n<li>ENSPRYNG is given by an injection under the skin (subcutaneously). If your healthcare provider decides that you or your caregiver can give your injections of ENSPRYNG, you or your caregiver should receive training on the right way to prepare and inject ENSPRYNG.</li>\n<li>Always inject all of the medicine in the syringe.</li>\n<li>The first 3 injections (loading period) of ENSPRYNG are taken 1 time every 2 weeks.</li>\n<li>After this, injection of ENSPRYNG is taken every 4 weeks (maintenance period). Keep taking ENSPRYNG 1 time every 4 weeks for as long as your healthcare provider tells you to.</li>\n<li>If you miss a dose of ENSPRYNG, talk to your health care provider about restarting dosing.</li>\n</ul>\n</td>\n</tr>\n<tr>\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\"><a name=\"whatare\"></a>What are the possible side effects of ENSPRYNG?<br/>ENSPRYNG may cause serious side effects, including:</span>\n<ul>\n<li>See <span class=\"Bold\">\"<a href=\"#whatis\">What is the most important information I should know about ENSPRYNG?</a>\"</span>\n</li>\n<li>\n<span class=\"Bold\">Serious allergic reactions.</span> Serious allergic reactions that may be life-threatening have happened with other medicines like ENSPRYNG. Tell your healthcare provider before taking your next dose if you had hives, rash, or flushing after your injection. Seek medical attention right away if you have any symptoms of a serious allergic reaction, such as:</li>\n</ul>\n</td>\n</tr>\n<tr>\n<td align=\"left\" class=\"Lrule\"></td><td align=\"left\">\n<ul class=\"Circle\">\n<li>shortness of breath or trouble breathing </li>\n<li>dizziness or feeling faint</li>\n</ul>\n</td><td align=\"left\" class=\"Rrule\">\n<ul class=\"Circle\">\n<li>swelling of your lips, face, or tongue</li>\n<li>moderate or severe stomach (abdominal) pain or vomiting</li>\n<li>chest pain</li>\n</ul>\n</td>\n</tr>\n<tr>\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\">\n<ul>\n<li>The most common side effects of ENSPRYNG include:</li>\n</ul>\n</td>\n</tr>\n<tr>\n<td align=\"left\" class=\"Lrule\"></td><td align=\"left\">\n<ul class=\"Circle\">\n<li>sore throat, runny nose (nasopharyngitis)</li>\n<li>rash</li>\n<li>fatigue</li>\n<li>extremity pain</li>\n</ul>\n</td><td align=\"left\" class=\"Rrule\">\n<ul class=\"Circle\">\n<li>headache</li>\n<li>upper respiratory tract infection</li>\n<li>nausea</li>\n<li>inflammation of the stomach lining (gastritis)</li>\n<li>joint pain</li>\n</ul>\n</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\">These are not all the possible side effects of ENSPRYNG.<br/>Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800-FDA-1088. You may also report side effects to Genentech at 1-888-835-2555.</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">How should I store ENSPRYNG?</span>\n<ul>\n<li>Store ENSPRYNG in the refrigerator between 36°F to 46°F (2°C to 8°C) in the original carton.</li>\n<li>Protect from light.</li>\n<li>\n<span class=\"Bold\">Do not</span> freeze or use the syringe if it has been frozen.</li>\n<li>\n<span class=\"Bold\">Do not</span> shake.</li>\n<li>ENSPRYNG, if unopened, can be removed from and returned to the refrigerator, if needed. The total combined time out of the refrigerator should not be more than 8 days at a temperature that does not go above 86°F (30°C).</li>\n</ul>\n</td>\n</tr>\n<tr class=\"Botrule\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\">General information about the safe and effective use of ENSPRYNG.</span>\n<br/>Medicines are sometimes prescribed for purposes other than those listed in a <a href=\"#MG\">Medication Guide</a>. Do not use ENSPRYNG for a condition for which it was not prescribed. Do not give ENSPRYNG to other people, even if they have the same symptoms that you have. It may harm them. You can ask your pharmacist or healthcare provider for information about ENSPRYNG that is written for health professionals.</td>\n</tr>\n<tr class=\"Last\">\n<td align=\"left\" class=\"Lrule Rrule\" colspan=\"3\"><span class=\"Bold\"><a name=\"ingredients\"></a>What are the ingredients in ENSPRYNG?</span>\n<br/>\n<span class=\"Bold\">Active ingredient:</span> satralizumab-mwge<br/>\n<span class=\"Bold\">Inactive ingredients:</span> L-arginine, L-histidine, poloxamer 188, L-aspartic acid, and Water for Injection.<br/>Manufactured by: <span class=\"Bold\">Genentech, Inc.</span>, A Member of the Roche Group, 1 DNA Way, South San Francisco, CA 94080-4990<br/>ENSPRYNG<span class=\"Sup\">®</span> is a registered trademark of Chugai Pharmaceutical Co., Ltd., Tokyo, Japan<br/>U.S. License No.: 1048<br/>For more information, go to www.ENSPRYNG.com or call 1-844-NSPRYNG.</td>\n</tr>\n</tbody>\n</table></div>" }

Read this Instructions for Use before you start using your prefilled syringe and each time you get a refill. There may be new information. This information does not take the place of talking to your healthcare provider about your medical condition or treatment. Your healthcare provider will decide if you or a caregiver can give you injections of ENSPRYNG at home. They will also show you or a caregiver the correct and safe way to use the syringe before you use it for the first time.

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Talk to your healthcare provider if you have any questions.

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Important Information

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Do not share your ENSPRYNG syringe with other people. You may give them a serious infection or get a serious infection from them.

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Do not:

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How should I store the ENSPRYNG prefilled syringe?

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Keep the ENSPRYNG syringe and all medicines out of the reach of children.

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Do not:

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Supplies needed to give your injection

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Each ENSPRYNG carton contains:

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Not included in the carton:

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ENSPRYNG prefilled syringe(See Figure A and Figure B)Before use:

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After use:

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The syringe has a needle-shield that automatically covers the needle when the injection is complete.

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Prepare to use ENSPRYNG

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If the expiration date has passed or the seal is broken, do not use. Then go to Step 21 "Disposing of ENSPRYNG" and contact your healthcare provider.

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Check the syringe

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(See Figure F)

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If the expiration (EXP) date has passed, the syringe is damaged or the liquid is cloudy, discolored or has particles in it, do not use. Then go to Step 21 "Disposing of ENSPRYNG" and contact your healthcare provider.

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Let your syringe warm up

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Wash your hands

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Choose the injection site

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Choose a different injection site for each new injection. Choose a different place to inject which is at least 1 inch (2.5 cm) away from the place where you last injected.

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Clean the injection site

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Inject ENSPRYNG

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Taking care of the injection site

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Disposing of ENSPRYNG

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This Instructions for Use has been approved by the U.S. Food and Drug Administration.

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Manufactured by: Genentech, Inc. A Member of the Roche Group1 DNA WaySouth San Francisco, CA 94080-4990

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U.S. License No.: 1048

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Approved: 8/2020

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ENSPRYNG® is a registered trademark of Chugai Pharmaceutical Co., Ltd., Tokyo, Japan

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© 2020 Genentech, Inc. All rights reserved.

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Representative sample of labeling (see the HOW SUPPLIED section for complete listing):

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NDC 50242-007-01

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Rx only

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Enspryng® (satralizumab-mwge)Injection

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120 mg/mL

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For Subcutaneous Use.Single-Dose Prefilled Syringe.

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Refrigerate at 2°C to 8°C (36°F to 46°F) in original carton to protect from light.Do not freeze. Do not shake.

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ATTENTION PHARMACIST: Each patient is required to receive the enclosedMedication Guide.

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1 prefilled syringe

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Genentech

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10240933

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