POLICY REVIEW CYCLE
Effective Date
|
Date of Origin
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04-01-2024
|
|
FDA APPROVED INDICATIONS AND DOSAGE
Agent(s)
|
FDA Indication(s)
|
Notes
|
Ref#
|
Berinert®
(C1 esterase inhibitor, [human])
Freeze-dried powder for reconstitution for intravenous use
|
Treatment of acute abdominal, facial, or laryngeal hereditary angioedema (HAE) attacks in adults and pediatric patients
The safety and efficacy of Berinert for prophylactic therapy has not been established.
|
|
1
|
CINRYZE®
(C1 esterase inhibitor, [human])
Lyophilized powder for reconstitution for intravenous use
|
Treatment for routine prophylaxis against angioedema attacks in adult, adolescents, and pediatric patients (6 years and older) with hereditary angioedema (HAE)
|
|
2
|
Firazyr®
(icatibant)*
Injection for subcutaneous use
|
Treatment of acute attacks of hereditary angioedema (HAE) in adults 18 years of age and older
|
*generic available
|
3
|
HAEGARDA®
(C1 esterase inhibitor [human])
Freeze-dried powder for reconstitution for subcutaneous injection
|
Routine prophylaxis to prevent Hereditary Angioedema (HAE) attacks in patients 6 years of age and older
|
|
4
|
Orladeyo®
(berotralstat)
Capsule
|
Prophylaxis to prevent attacks of hereditary angioedema (HAE) in adults and pediatric patients 12 years and older
Limitations of use: Orladeyo should not be used for treatment of acute attacks.
|
|
5
|
RUCONEST®
(C1 esterase inhibitor, [recombinant])
Lyophilized powder for reconstitution for intravenous use
|
Treatment of acute attacks of hereditary angioedema (HAE) in adults and adolescent patients with HAE
Limitations of use: Effectiveness was not established in HAE patients with laryngeal attacks.
|
|
6
|
TAKHZYRO®
(lanadelumab-flyo)
Injection solution for subcutaneous use
|
Prophylaxis to prevent attacks of hereditary angioedema (HAE) in adult and pediatric patients 2 years and older
|
|
7
|
See package insert for FDA prescribing information: https://dailymed.nlm.nih.gov/dailymed/index.cfm
CLINICAL RATIONALE
Hereditary Angioedema
|
Hereditary Angioedema (HAE) is an autosomal dominant disease. HAE is characterized by recurrent episodes/attacks of nonpruritic, nonpitting, subcutaneous or submucosal edema that may involve the extremities, bowels, genitalia, trunk, face, tongue, or larynx. Angioedema attacks typically lasts 3 to 5 days from start to resolution, with increased morbidity and mortality if not treated with effective medication. Lack of clinical efficacy in treating HAE symptoms with antihistamines, corticosteroids, or epinephrine, is an important indicator for diagnosis.(8,9)
HAE can be divided into two types, HAE due to C1INH deficiency (HAE-C1INH) and HAE with normal C1INH (HAE-nI-C1INH). HAE-C1INH can be subdivided into Type 1, characterized by deficient levels of C1 esterase inhibitor (C1-INH) protein and function, and Type 2, characterized by normal levels of C1-INH protein with diminished C1-INH activity (i.e., dysfunctional C1-INH protein). The prevalence of HAE-C1INH Type 1 and I2 is approximately 1 in 50,000 persons worldwide, and approximately 6000 affected individuals in the United States. HAE-C1INH Types 1 and 2 occur as a result of a mutation in the SERPING1 gene, which codes for C1-INH, and ultimately leads to the increased generation of bradykinin. Bradykinin has been credited in all HAE types for involvement in attacks through increasing vascular permeability via the B2 receptor.(8,9) HAE-nI-C1INH, previously referred to as Type 3 HAE, is characterized by both normal C1-INH protein and functional levels and may also be bradykinin mediated based on the lack of response to antihistamines, corticosteroids, and epinephrine, and the favorable response to bradykinin pathway-targeted medications.(8,9) HAE-nI-C1INH can be further subdivided into 5 subtypes:(8)
- HAE FXII: due to mutation in F12, the gene encoding coagulation FXII
- HAE-PLG: due to mutations in PLG, the gene encoding plasminogen
- HAE-ANGPT1: due to mutations in ANGPT1, the gene encoding angiopoietin-1
- HAE-KNG1: due to a mutation in kininogen1 gene
- HAE-unknown: patients for whom the responsible mutation has not yet been defined
The World Allergy Organization and European Academy of Allergy and Clinical Immunology (WAO/EAACI) recognize two additional subtypes of HAE-nI-C1INH. HAE-HS3ST6, which results from a mutation in the heparan sulfate 3-O-sulfotransferase 6 gene, and HAE-MYOF, which results from a mutation in the myoferlin gene.(9)
Symptoms of HAE-C1INH typically begin in the first or second decade of life (sometimes as young as 2 years of age) and persist throughout the patient’s lifetime. Almost all patients with HAE-C1INH will manifest symptoms by the age of 20.(8,9) An acute attack that causes death is most often a result of abdominal or laryngeal involvement. Triggers for attacks vary and may be traceable to a source (e.g., minor trauma or stress); however, episodes often occur without a defined precipitating factor.(9) HAE-nI-C1INH has a similar clinical presentation to HAE-C1INH with some differences. The face and tongue are more frequently affected, with fewer abdominal symptoms. While HAE-nI-C1INH is also an autosomal dominant disorder, penetrance is variable and often lower than patients with HAE-C1INH.(8,9)
In addition to clinical presentation and an assessment of family history, HAE diagnosis typically includes a laboratory workup of C4, C1-INH antigenic level, and C1-INH function. C4, the natural substrate for C1 esterase, is considered the single best screening test for C1-INH deficiency.(8,9) In order to further distinguish between Type 1 and Type 2 HAE, the C1-INH antigenic level and/or functional activity is measured. The 2017 update to the international consensus from WAO and the European Association of Allergy and Clinical Immunology recommend patients with suspected HAE should have blood levels of C1-INH function, C1-INH protein, and C4 assessed, and the tests should be repeated to confirm diagnosis of HAE Type 1 or 2. A diagnosis of Type 1 can be confirmed with a decrease in C1-INH function, C1-INH protein level, and C4 levels. A diagnosis of Type 2 can be confirmed with a decrease in C1-INH function and C4 level with an increase or normal level of C1-INH protein level.(9)
The US HAE Association Medical Advisory Board (2020) indicates further repeated testing is neither necessary nor useful once C1INH deficiency has been established by laboratory testing. The guidelines also recommend evaluating current medications that affect bradykinin and that can cause angioedema (e.g., angiotensin converting-enzyme inhibitors and estrogen replacement) and stopping these when appropriate. Genetic sequencing isn’t usually necessary to establish the diagnosis due to the high sensitivity and specificity of biochemical tests currently available. Genetic screening may be beneficial in prenatal testing, when biochemical testing is repeatedly equivocal, or to differentiate between HAE-C1INH and acquired C1INH. The board also recommends that patients see prescribers that are HAE experts to optimize individual treatment plans, assist with coordinating care, and provide important patient and family education.(8)
HAE-nI-C1INH does not have validated biochemical testing to confirm the diagnosis. Genetic testing may be more helpful in confirming HAE-nI-C1INH for the subtypes with common mutations. The diagnosis of HAE-nI-C1INH can be suspected in patients with normal C1INH levels and the presence of angioedema. Genetic tests for factor XII, plasminogen, angiopoetin-1, and kininogen1 should be performed when available. A diagnosis of HAE-U should involve input from an HAE specialist.(8)
On-Demand Treatment Recommendations
The 2021 update to the international consensus from WAO/EAACI and the US HAE Association Medical Advisory Board 2020 indicate that all patients with laboratory confirmed HAE-C1INH should have at least two standard doses of an FDA approved on-demand treatment for acute attacks.(8,9) Currently, clinical evidence supporting the use of more than one agent used to treat acute attacks at the same time is lacking. The 2021 update to the international consensus from WAO/EAACI recommend all HAE-C1INH attacks considered for on-demand therapy be treated with either C1-INH, ecallantide, or icatibant.(9)
US HAE Association Medical Advisory Board 2020 recommends early treatment options of acute attacks for HAE-C1INH and HAE-nI-C1INH consist of plasma derived nanofiltered C1-INH (Berinert), recombinant human C1-INH (Ruconest), ecallantide (Kalbitor), icatibant (Firazyr), or fresh frozen plasma. The medication selection should be individualized based on patient response and all attacks should be considered for treatment irrespective of anatomical location. Patients that self-administer treatment should seek medical care if the features of their attack are unusual, response to treatment is inadequate, or they experience an airway attack. Fresh frozen plasma can be used if none of the FDA-approved on-demand treatments are available. The Board notes that numerous open-labeled reports have revealed successful responses of each of the on-demand treatment for HAE-n1-C1INH attacks.(8)
Short-Term Prophylaxis Recommendations
Patients may need prophylactic treatment prior to planned surgeries or procedures, particularly dental surgeries. Trauma and/or stress are well-known provocateurs of acute attacks.(8) The 2021 update to the international consensus from WAO/EAACI recommends that short-term prophylaxis should be used prior to procedures that can induce an attack. C1-INH should be used as close as possible to the start of the procedure. Second-line options for short-term prophylaxis include fresh frozen plasma and androgens, but neither have the safety or efficacy of intravenous C1-INH.(9)
US HAE Association Medical Advisory Board 2020 recommends the following:(8)
- HAE-C1INH:
- Short-term prophylaxis can be either a single dose of plasma derived C1INH [pdC1INH (CINRYZE, HAEGARDA)] or a course of anabolic androgen
- A single dose of 20 IU/kg pdC1INH can be given 1 to 12 hours before the stressor
- Anabolic androgens (i.e., danazol at 400 to 600 mg/day) can be administered 5-7 days before procedure or stressor and continued for 2-5 days after
- Recombinant human C1INH [rhC1INH (RUCONEST)] at 50 IU/kg has also been successfully used for short-term prophylaxis
- On-demand treatment needs to be available regardless of use of short-term prophylaxis
- HAE-nI-C1INH:
- There is no data on short-term prophylaxis
- For patients with a confirmed diagnosis, the same approach as HAE-C1INH may be used with the important caveat that on-demand therapy be available if needed
Long-Term Prophylaxis Recommendations
The 2021 update to the international consensus from WAO/EAACI recommends the following:(9)
- Long-term prophylaxis should be considered for all severely symptomatic patients, taking into account the disease activity, frequency of attacks, quality of life, availability of health care resources, and failure to achieve adequate control with appropriate on-demand therapy
- All patients should be evaluated for prophylaxis at least once a year or during every office visit, and once started, efficacy and safety of long-term prophylaxis should be assessed regularly
- Plasma-derived C1-INH, lanadelumab, and berotralstat are recommended as first-line therapy and androgens are second-line therapy
- Antifibrinolytics are not recommended for long-term prophylaxis
US HAE Association Medical Advisory Board 2020 recommends the following:(8)
- HAE-C1INH
- Long-term prophylaxis should be individualized and consider attack severity, frequency, comorbid conditions, and patient experience/preference.
- Medication options can be divided into two broad categories: first-line and second-line
- First-line options include C1-INH (IV CINRYZE and SC HAEGARDA), and a monoclonal inhibitor of plasma kallikrein (TAKHZYRO)
- Second-line options include anabolic androgens (i.e., danazol) and antifibrinolytics (epsilon aminocaproic acid or tranexamic acid)
- Second-line options should be reserved for when first-line agents are not available or when the patient will only accept oral therapy
- HAE-nI-C1INH:
- Long-term prophylaxis has not been studied in patients with HAE-nI-C1INH
- There are 2 strategies frequently used for prophylaxis in patients with HAE-nI-C1INH: hormonal therapy and antifibrinolytics
- Monitoring:
- Attack frequency and severity should be evaluated by the physician on an ongoing basis
- The US HAEA MAB recommends that patients keep a record of all of their attacks, regardless of severity (mild, moderate, or severe). These records should include description of attack, treatment of attack, response to treatment, and any adverse effects of treatment.
- The attack log should be provided to the treating physicians and reviewed on a regular basis by a means (i.e., in person or electronically) predetermined between the patient and the physician
- When patients self-administer or receive on-demand medications, there must be a plan to have the patient report this use in a timely manner
- The HAE MAB recommends that potential triggers, an updated list of current medications, to ensure that patients are not taking an angiotensin-converting enzyme inhibitor or estrogen replacement, and immunizations be reviewed when patients come into the office for visits
There are currently two C1-INH that are approved for prophylaxis, HAEGARDA and CINRYZE, and one kallikrein inhibitor that is approved for prophylaxis, TAKHZYRO. The clinical trials for HAEGARDA and TAKHZYRO included patients with a pretreatment attack rate of 3.3 and 3.5 attacks per month. The clinical trials for CINRYZE required patients to have at least 2 attacks per month. The Institute for Clinical and Economic Review (ICER) completed a cost-comparison review of the three prophylaxis agents against on-demand therapy. It was found that the prophylaxis would be more cost effective for patients experiencing 3.3 attacks or more per month, while the on-demand treatment(s) would be more cost effective for patients experiencing fewer than 3.3 attacks per month.(11)
ICER completed a Real-World Evaluation of the prophylactic agents, noting a decrease in severe attack rates for CINRYZE, HAEGARDA, and TAKHZYRO with rates similar to those noted in clinical trials. A separate analysis of TAKHZYRO showed 64% of patients that initiated therapy with TAKHZYRO achieved an attack free status during the first 6 months of therapy. Of those that were attack free, 74% had a dose reduction to every 4 weeks.(12)
Special Population Recommendations:
The 2021 update to the international consensus from WAO/EAACI recommend the following for children and pregnant women with HAE:(9)
- C1-INH is recommended as first-line therapy for acute attacks, short-term and long-term prophylaxis in children, pregnancy, and lactation. C1-INH is considered safe and effective during pregnancy and lactation.
- Attenuated androgens can be used second-line for short-term prophylaxis in children when C1-INH is unavailable. US HAE Association Medical Advisory Board 2020 does NOT recommend the use of androgens for use in children.(8)
- Antifibrinolytics are preferred to androgens as second-line therapy for long-term prophylaxis in children
- Androgens and antifibrinolytics are secreted in breast milk and in contrast to androgens, tranexamic acid was found to be safe during breastfeeding
|
Efficacy
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TAKHZYRO(7)
The efficacy of TAKHZYRO for the prevention of angioedema attacks in patients 12 years of age and older with Type I or II HAE was demonstrated in a multicenter, randomized, double-blind, placebo-controlled parallel-group study (Trial 1, NCT02586805).
The study included 125 adult and pediatric patients (12 years of age and older) with Type I or II HAE who experienced at least one investigator-confirmed attack per 4 weeks during the run-in period. Patients were randomized into 1 of 4 parallel treatment arms, stratified by baseline attack rate, in a 3:2:2:2 ratio (placebo, lanadelumab-flyo 150 mg every 4 weeks, lanadelumab-flyo 300 mg every 4 weeks, or lanadelumab-flyo 300 mg every 2 weeks by subcutaneous injection) for the 26-week treatment period. Patients 18 years of age and older were required to discontinue other prophylactic HAE medications prior to entering the study; however, all patients were allowed to use rescue medications for treatment of breakthrough HAE attacks.
All TAKHZYRO treatment arms produced clinically meaningful and statistically significant reductions in the mean HAE attack rate compared to placebo across all primary and secondary endpoints in the Intent-to-Treat population (ITT).
Endpoint statistics
|
Placebo (N=41)
|
TAKHZYRO 150 mg every 4 weeks
|
TAKHZYRO 300 mg every 4 weeks
|
TAKHZYRO 300 mg every 2 weeks
|
Number of HAE attacks from day 0 to day 182
|
Least squares mean (95% CI) monthly attack rate (attacks/4 weeks)
|
1.97
(1.64, 2.36)
|
0.48
(0.31, 0.73)
|
0.53
(0.36, 0.77)
|
0.26
(0.14, 0.46)
|
% reduction relative to placebo (95% CI)
|
|
76 (61, 85)
|
73 (59, 82)
|
87 (76, 93)
|
Adjusted p-values
|
|
<0.001
|
<0.001
|
<0.001
|
Number of HAE attacks requiring acute treatment from day 0 to day 182
|
Least squares mean (95% CI) monthly attack rate (attacks/4 weeks)
|
1.64
(1.34, 2.00)
|
0.31
(0.18, 0.53)
|
0.42
(0.28, 0.65)
|
0.21
(0.11, 0.40)
|
% reduction relative to placebo (95% CI)
|
|
81 (66, 89)
|
74 (59, 84)
|
87 (75, 93)
|
Adjusted p-values
|
|
<0.001
|
<0.001
|
<0.001
|
Number of moderate or severe HAE attacks from day 0 to day 182
|
Least squares mean (95% CI) monthly attack rate (attacks/4 weeks)
|
1.22
(0.97, 1.52)
|
0.36
(0.22, 0.58)
|
0.32
(0.20, 0.53)
|
0.20
(0.11, 0.39)
|
% reduction relative to placebo (95% CI)
|
|
70 (50, 83)
|
73 (54, 84)
|
83 (67, 92)
|
Adjusted p-values
|
|
<0.001
|
<0.001
|
<0.001
|
The mean reduction in HAE attack rate was consistently higher across the TAKHZYRO treatment arms compared to placebo regardless of the baseline history of prior long-term prophylaxis, laryngeal attacks, or attack rate during the run-in period.
Additional pre-defined exploratory endpoints included the percentage of patients who were attack free for the entire 26-week treatment period and the percentage of patients achieving threshold (greater than or equal to 50%, greater than or equal to 70%, greater than or equal to 90%) reductions in HAE attack rates compared to run-in during the 26-week treatment period. A 50% or greater reduction in HAE attack rates was observed in 100% of patients on 300 mg every 2 weeks or every 4 weeks and 89% on 150 mg every 4 weeks compared to 32% of placebo patients. A 70% or greater reduction in HAE attack rates was observed in 89%, 76%, and 79% of patients on 300 mg every 2 weeks, 300 mg every 4 weeks, and 150 mg every 4 weeks, respectively, compared to 10% of placebo patients. A 90% or greater reduction in HAE attack rates was observed 67%, 55%, and 64% of patients on 300 mg every 2 weeks, 300 mg every 4 weeks, and 150 mg every 4 weeks, respectively, compared to 5% of placebo patients.
The percentage of attack-free patients for the entire 26-week treatment period was 44%, 31%, and 39% in the TAKHZYRO 300 mg every 2 weeks, 300 mg every 4 weeks, and 150 mg every 4 weeks groups respectively, compared to 2% of placebo patients.
Trial 2 (NCT02741596) is a rollover into an open-label extension study. Patients that completed Trial 1 were eligible to be rolled over regardless of randomization in Trial 1. Patients received a single dose of TAKHZYRO 300 mg at study entry and were followed until the first HAE attack occurred. All efficacy endpoints were exploratory in this uncontrolled, unblinded study. At week 4 post-dose, approximately 80% of patients who had been in the 300 mg every 2 weeks treatment group (N=25) in Trial 1 remained attack-free. After the first HAE attack, all patients received open-label treatment with TAKHZYRO 300 mg every 2 weeks.
|
Safety
|
Berinert, CINRYZE, and HAEGARDA are contraindicated in patients with a history life-threatening hypersensitivity reactions, including anaphylaxis, to C1-INH preparations or its excipients.(1,2,4)
RUCONEST is contraindicated in patients with the following:(6)
- History of allergy to rabbits or rabbit-derived products
- History of immediate hypersensistivity reactions, including anaphylaxis, to C1 esterase inhibitor preparations
Firazyr, Orladeyo, and TAKHZYRO have no FDA labeled contraindications for use.(3,5,7)
|
REFERENCES
Number
|
Reference
|
1
|
Berinert prescribing information. CSL Behring GmbH. September 2021.
|
2
|
CINRYZE prescribing information. Takeda Pharmaceuticals America, Inc. February 2023.
|
3
|
Firazyr prescribing information. Takeda Pharmaceuticals America, Inc. October 2021.
|
4
|
HAEGARDA prescribing information. CSL Behring GmbH. January 2022.
|
5
|
Orladeyo prescribing information. BioCryst Pharmaceuticals, Inc. December 2020.
|
6
|
RUCONEST prescribing information. Bioconnection B.V. April 2020.
|
7
|
TAKHZYRO prescribing information. Takeda Pharmaceuticals America, Inc. February 2023.
|
8
|
Busse PJ, Christiansen SC, Riedl MA, Banerji A, Bernstein JA, Castaldo AJ, Craig T, Davis-Lorton M, Frank MM, Li HH, Lumry WR, Zuraw BL. US HAEA Medical Advisory Board 2020 Guidelines for the Management of Hereditary Angioedema. J Allergy Clin Immunol in Pract. 2021 Jan;9(1):132-150.E3. doi:10.1016/j.jaip.2020.08.046.
|
9
|
Maurer M, Magerl M, Betschel S, et al. The international WAO/EAACI guideline for the management of hereditary angioedema - The 2021 revision and update. Allergy. July 2022; 77(7):1961-1990. doi:10.1111/all.15214
|
10
|
Fryar, Cheryl D.;Carroll, Margaret D.;Gu, Qiuping;Afful, Joseph;Ogden, Cynthia L. CDC. Anthropometric reference data for children and adults:United States, 2015-2018. Vital and health statistics. Series 3, Analytical and epidemiological studies;no. 46. January 2021. https://stacks.cdc.gov/view/cdc/100478
|
11
|
Institute for Clinical and Economic Review (ICER). Prophylaxis for Hereditary Angioedema with Lanadelumab and C1 Inhibitors: Effectiveness and Value. Final Evidence Report. November 15, 2018.
|
12
|
Bloudek L, Jaksa A, McKenna A, Carlson J, Chen Y, Patrick A, Campbell JD. Observational Real-World Evidence Update; Prophylaxis of Hereditary Angioedema with Takhzyro and C1 Inhibitors: Effectiveness and Value. August 24, 2021. https://icer.org/assessment/hereditary-angioedema-2018/#timeline
|
POLICY AGENT SUMMARY PRIOR AUTHORIZATION
Target Brand Agent(s)
|
Target Generic Agent(s)
|
Strength
|
Targeted MSC
|
Available MSC
|
Final Age Limit
|
Preferred Status
|
|
Orladeyo
|
berotralstat hcl cap
|
110 MG ; 150 MG
|
M ; N ; O ; Y
|
N
|
|
|
Cinryze ; Haegarda
|
c1 esterase inh
|
2000 UNIT ; 3000 UNIT ; 500 UNIT
|
M ; N ; O ; Y
|
N
|
|
|
Berinert
|
c1 esterase inh
|
500 UNIT
|
M ; N ; O ; Y
|
N
|
|
|
Ruconest
|
c1 esterase inh
|
2100 UNIT
|
M ; N ; O ; Y
|
N
|
|
|
Firazyr ; Sajazir
|
icatibant acetate subcutaneous soln pref syr
|
30 MG/3ML
|
M ; N ; O ; Y
|
O ; Y
|
|
|
Takhzyro
|
lanadelumab-flyo inj
|
300 MG/2ML
|
M ; N ; O ; Y
|
N
|
|
|
Takhzyro
|
lanadelumab-flyo soln pref syringe
|
150 MG/ML ; 300 MG/2ML
|
M ; N ; O ; Y
|
N
|
|
|
POLICY AGENT SUMMARY QUANTITY LIMIT
Target Brand Agent Name(s)
|
Target Generic Agent Name(s)
|
Strength
|
QL Amount
|
Dose Form
|
Day Supply
|
Duration
|
Addtl QL Info
|
Allowed Exceptions
|
Targeted NDCs When Exclusions Exist
|
|
Berinert
|
C1 Esterase Inhibitor (Human) For IV Inj Kit 500 Unit
|
500 UNIT
|
10
|
Vials
|
30
|
DAYS
|
based on CDC 90th percentile for men and women averaged to 247.5 lbs or 112.5 kg (112.5 kg * 20 IU/kg=2,250 IU/500 IU/bottle=4.5 or 5 bottles or 2500 units/attack x 2 attacks/month = 10 vials/28 days
|
|
|
Cinryze
|
C1 Esterase Inhibitor (Human) For IV Inj 500 Unit
|
500 UNIT
|
20
|
Vials
|
30
|
DAYS
|
1,000 IU every 3 days = 10,000 IU/30 days/500 u/vial = 20 vials
|
|
|
Firazyr ; Sajazir
|
icatibant acetate subcutaneous soln pref syr
|
30 MG/3ML
|
6
|
Syringes
|
30
|
DAYS
|
|
|
|
Haegarda
|
C1 Esterase Inhibitor (Human) For Subcutaneous Inj 2000 Unit
|
2000 UNIT
|
27
|
Vials
|
28
|
DAYS
|
*QL calculation based on CDC 90 percentile for weight in adults, averaged for men and women, and rounded to the nearest even dose to reduce waste (112.5 kg individual). See Special Clinical Criteria Table ** Do not wildcard PA- detail to GPI 14
|
|
|
Haegarda
|
C1 Esterase Inhibitor (Human) For Subcutaneous Inj 3000 Unit
|
3000 UNIT
|
18
|
Vials
|
28
|
DAYS
|
*QL calculation based on CDC 90 percentile for weight in adults, averaged for men and women, and rounded to the nearest even dose to reduce waste (112.5 kg individual). See Special Clinical Criteria Table ** Do not wildcard PA- detail to GPI 14
|
|
|
Orladeyo
|
berotralstat hcl cap
|
110 MG ; 150 MG
|
30
|
Capsules
|
30
|
DAYS
|
|
|
|
Ruconest
|
C1 Esterase Inhibitor (Recombinant) For IV Inj 2100 Unit
|
2100 UNIT
|
8
|
Vials
|
30
|
DAYS
|
|
|
|
Takhzyro
|
Lanadelumab-flyo Inj 300 MG/2ML (150 MG/ML)
|
300 MG/2ML
|
2
|
Vials
|
28
|
DAYS
|
|
|
|
Takhzyro
|
lanadelumab-flyo soln pref syringe
|
150 MG/ML
|
2
|
Syringes
|
28
|
DAYS
|
|
|
|
Takhzyro
|
lanadelumab-flyo soln pref syringe
|
300 MG/2ML
|
2
|
Syringes
|
28
|
DAYS
|
|
|
|
ADDITIONAL QUANTITY LIMIT INFORMATION
Wildcard
|
Target Brand Agent Name(s)
|
Target Generic Agent Name(s)
|
Strength
|
Additional QL Information
|
Targeted NDCs When Exclusions Exist
|
Effective Date
|
Term Date
|
|
85802022006420
|
Berinert
|
C1 Esterase Inhibitor (Human) For IV Inj Kit 500 Unit
|
500 UNIT
|
based on CDC 90th percentile for men and women averaged to 247.5 lbs or 112.5 kg (112.5 kg * 20 IU/kg=2,250 IU/500 IU/bottle=4.5 or 5 bottles or 2500 units/attack x 2 attacks/month = 10 vials/28 days
|
|
|
|
85802022002120
|
Cinryze
|
C1 Esterase Inhibitor (Human) For IV Inj 500 Unit
|
500 UNIT
|
1,000 IU every 3 days = 10,000 IU/30 days/500 u/vial = 20 vials
|
|
|
|
85802022002130
|
Haegarda
|
C1 Esterase Inhibitor (Human) For Subcutaneous Inj 2000 Unit
|
2000 UNIT
|
*QL calculation based on CDC 90 percentile for weight in adults, averaged for men and women, and rounded to the nearest even dose to reduce waste (112.5 kg individual). See Special Clinical Criteria Table ** Do not wildcard PA- detail to GPI 14
|
|
|
|
85802022002140
|
Haegarda
|
C1 Esterase Inhibitor (Human) For Subcutaneous Inj 3000 Unit
|
3000 UNIT
|
*QL calculation based on CDC 90 percentile for weight in adults, averaged for men and women, and rounded to the nearest even dose to reduce waste (112.5 kg individual). See Special Clinical Criteria Table ** Do not wildcard PA- detail to GPI 14
|
|
|
|
CLIENT SUMMARY – PRIOR AUTHORIZATION
Target Brand Agent Name(s)
|
Target Generic Agent Name(s)
|
Strength
|
Client Formulary
|
Berinert
|
c1 esterase inh
|
500 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Cinryze ; Haegarda
|
c1 esterase inh
|
2000 UNIT ; 3000 UNIT ; 500 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Firazyr ; Sajazir
|
icatibant acetate subcutaneous soln pref syr
|
30 MG/3ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Orladeyo
|
berotralstat hcl cap
|
110 MG ; 150 MG
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Ruconest
|
c1 esterase inh
|
2100 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Takhzyro
|
lanadelumab-flyo inj
|
300 MG/2ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Takhzyro
|
lanadelumab-flyo soln pref syringe
|
150 MG/ML ; 300 MG/2ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
CLIENT SUMMARY – QUANTITY LIMITS
Target Brand Agent Name(s)
|
Target Generic Agent Name(s)
|
Strength
|
Client Formulary
|
Berinert
|
C1 Esterase Inhibitor (Human) For IV Inj Kit 500 Unit
|
500 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Cinryze
|
C1 Esterase Inhibitor (Human) For IV Inj 500 Unit
|
500 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Firazyr ; Sajazir
|
icatibant acetate subcutaneous soln pref syr
|
30 MG/3ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Haegarda
|
C1 Esterase Inhibitor (Human) For Subcutaneous Inj 2000 Unit
|
2000 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Haegarda
|
C1 Esterase Inhibitor (Human) For Subcutaneous Inj 3000 Unit
|
3000 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Orladeyo
|
berotralstat hcl cap
|
110 MG ; 150 MG
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Ruconest
|
C1 Esterase Inhibitor (Recombinant) For IV Inj 2100 Unit
|
2100 UNIT
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Takhzyro
|
Lanadelumab-flyo Inj 300 MG/2ML (150 MG/ML)
|
300 MG/2ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Takhzyro
|
lanadelumab-flyo soln pref syringe
|
150 MG/ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
Takhzyro
|
lanadelumab-flyo soln pref syringe
|
300 MG/2ML
|
Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx
|
PRIOR AUTHORIZATION CLINICAL CRITERIA FOR APPROVAL
Module
|
Clinical Criteria for Approval
|
Berinert, Firazyr, icatibant, or Ruconest
|
Initial Evaluation
Target Agent(s) will be approved when ALL of the following are met:
- ONE of the following:
- The patient has a diagnosis of hereditary angioedema (HAE) due to C1INH deficiency [HAE-C1INH (Type 1 or Type 2)] confirmed by ONE of the following:
- The patient’s diagnosis has been confirmed with measurements of C1-INH antigenic level, C1-INH functional level, and C4 level as follows:
- Type 1 HAE: Decreased quantities of C4 level, C1-INH antigenic level, and C1-INH functional level AND ONE of the following:
- The patient has a family history of HAE OR
- Acquired angioedema has been ruled out (i.e., patient onset of symptoms occur prior to 30 years old, normal C1q levels, patient does not have underlying disease such as lymphoma or benign monoclonal gammopathy [MGUS], etc) OR
- Type 2 HAE: Decreased quantities of C4 level and C1-INH functional level (C1-INH antigenic level may be normal or elevated) OR
- The patient’s diagnosis has been confirmed by mutation in the C1-INH gene altering protein synthesis and/or function OR
- The patient has a diagnosis of hereditary angioedema (HAE) with normal C1INH (HAE-nI-C1INH) (also known as HAE III) evidenced by ALL of the following:
- The patient has levels within the normal range for C1-INH antigenic level, C1-INH functional level, and C4 level AND
- Repeat blood testing during an attack has confirmed the patient does not have abnormal lab values indicative of Type 1 HAE or Type 2 HAE AND
- ONE of the following:
- The patient has a known HAE-causing mutation (e.g., mutation of coagulation factor FXII gene [F12 mutation], mutation in the angiopoietin-1 gene, mutation in the plasminogen gene, mutation in the kininogen 1 gene, mutation in the myoferlin gene, mutation in the heparan sulfate 30-O-sulfotransferase 6 gene, etc.) OR
- The patient has a family history of HAE and documented evidence of lack of efficacy of chronic high-dose antihistamine therapy (e.g., cetirizine standard dosing at up to four times daily or an alternative equivalent, given for at least one month or an interval long enough to expect three or more angioedema attacks) AND corticosteroids AND
- If the patient has an FDA approved indication, then ONE of the following:
- The patient’s age is within FDA labeling for the requested indication for the requested agent OR
- The prescriber has provided information in support of using the requested agent for the patient’s age for the requested indication AND
- The patient has a history of at least ONE of the following:
- Moderate to severe cutaneous attacks (without concomitant hives) OR
- Abdominal attacks OR
- Mild to severe airway swelling attacks of HAE (i.e., debilitating cutaneous/gastrointestinal symptoms OR laryngeal/pharyngeal/tongue swelling) AND
- Medications known to cause angioedema (i.e., ACE-Inhibitors, estrogens, angiotensin II receptor blockers, dipeptidyl peptidase IV [DPP-IV] inhibitors, neprilysin inhibitors) have been evaluated and discontinued when appropriate AND
- The requested agent will be used to treat acute HAE attacks AND
- If the request is for one of the following brand agent(s) with an available generic equivalent (listed below), then ONE of the following:
Brand
|
Generic Equivalent
|
Firazyr
|
icatibant
|
- The patient has an intolerance or hypersensitivity to the generic equivalent that is not expected to occur with the brand agent OR
- The patient has an FDA labeled contraindication to the generic equivalent that is not expected to occur with the brand agent OR
- The prescriber has provided information to support the use of the brand agent over the generic equivalent AND
- The prescriber is a specialist in the area of the patient’s diagnosis (e.g., allergist, immunologist, hematologist, pulmonologist, medical geneticist) or the prescriber has consulted with a specialist in the area of the patient’s diagnosis AND
- ONE of the following:
- The patient will NOT be using the requested agent in combination with another agent indicated for the treatment of acute HAE attacks (i.e., Berinert, Firazyr, icatibant, Kalbitor, Ruconest) OR
- The prescriber has submitted documentation and justification for a second acute agent to be approved for up to a one month supply in a 12 month period AND
- The patient does NOT have any FDA labeled contraindications to the requested agent
Length of Approval: 6 months for first acute agent for HAE attacks, up to 1 month for second acute agent for HAE attacks
NOTE: If Quantity Limit applies, please refer to Quantity Limit Criteria.
*Step therapy requirement may not apply if a prior health plan paid for the medication - documentation of a paid claim may be required.
Renewal Evaluation
Target Agent(s) will be approved when ALL of the following are met:
- The patient has been previously approved for the requested agent through the plan’s Prior Authorization process AND
- The prescriber is a specialist in the area of the patient’s diagnosis (e.g., allergist, immunologist) or the prescriber has consulted with a specialist in the area of the patient’s diagnosis AND
- The patient has had clinical benefit with the requested agent AND
- If the request is for one of the following brand agent(s) with an available generic equivalent (listed below), then ONE of the following:
Brand
|
Generic Equivalent
|
Firazyr
|
icatibant
|
- The patient has an intolerance or hypersensitivity to the generic equivalent that is not expected to occur with the brand agent OR
- The patient has an FDA labeled contraindication to the generic equivalent that is not expected to occur with the brand agent OR
- The prescriber has provided information to support the use of the brand agent over the generic equivalent AND
- The prescriber has communicated (via any means) with the patient regarding frequency and severity of attacks and has verified that the patient does not have greater than 1-month supply (sufficient for 2 acute HAE attacks) currently on-hand AND
- If the patient is also on an agent for prophylaxis against HAE attacks, the prescriber has reduced the quantity of the acute agent one month after authorization of the prophylactic agent by at least 2 vials or 2 syringes and is continuing to assess acute agent use AND
- ONE of the following:
- The patient will NOT be using the requested agent in combination with another agent indicated for the treatment of acute HAE attacks (i.e., Berinert, Firazyr, icatibant, Kalbitor, Ruconest) OR
- The prescriber has submitted documentation and justification for a second acute agent to be approved for up to a one month supply in a 12 month period AND
- The patient does NOT have any FDA labeled contraindications to the requested agent
Length of Approval: 12 months for first acute agent for HAE attacks, up to 1 month for second acute agent for HAE attacks
NOTE: If Quantity Limit applies, please refer to Quantity Limit Criteria.
|
Cinryze, Haegarda, Orladeyo, or Takhzyro
|
Initial Evaluation
Target Agent(s) will be approved when ALL of the following are met:
- ONE of the following:
- The patient has a diagnosis of hereditary angioedema (HAE) due to C1INH deficiency [HAE-C1INH (Type 1 or Type 2)] evidenced by ONE of the following:
- The patient’s diagnosis has been confirmed with measurements of C1-INH antigenic level, C1-INH functional level, and C4 level as follows:
- Type 1 HAE: Decreased quantities of C4 level, C1-INH antigenic level, and C1-INH functional level OR
- Type 2 HAE: Decreased quantities of C4 level and C1-INH functional level (C1-INH antigenic level may be normal or elevated) OR
- The patient’s diagnosis has been confirmed by mutation in the C1-INH gene altering protein synthesis and/or function OR
- The patient has a diagnosis of hereditary angioedema (HAE) with normal C1INH (HAE-nI-C1INH) (formerly known as HAE III)] evidenced by ALL of the following:
- The patient has levels within the normal range for C1-INH antigenic level, C1-INH functional level, and C4 level AND
- Repeat blood testing during an attack has confirmed the patient does not have abnormal lab values indicative of HAE I or HAE II AND
- ONE of the following:
- The patient has a known HAE-causing mutation (e.g., mutation of coagulation factor XII gene [F12 mutation], mutation in the angiopoietin-1 gene, mutation in the plasminogen gene, etc.) OR
- The patient has a family history of HAE and documented evidence of lack of efficacy of chronic high-dose antihistamine therapy (e.g., cetirizine standard dosing at up to four times daily or an alternative equivalent, given for at least one month or an interval long enough to expect three or more angioedema attacks) AND corticosteroids AND
- The patient had an inadequate response or intolerance to an adequate trial of prophylactic therapy with an antifibrinolytic agent (e.g., tranexamic acid (TXA) or aminocaproic acid) and/or a 17α-alkylated androgen (e.g., danazol) unless contraindicated AND
- If the patient has an FDA approved indication, then ONE of the following:
- The patient’s age is within FDA labeling for the requested indication for the requested agent OR
- The prescriber has provided information in support of using the requested agent for the patient’s age for the requested indication AND
- ONE of the following:
- The requested agent is Cinryze and will be used to treat acute HAE attacks AND ONE of the following:
- The patient will NOT be using the requested agent in combination with another agent indicated for the treatment of acute HAE attacks OR
- The prescriber has submitted documentation and justification for a second acute agent to be approved for up to a one month supply in a 12 month period OR
- The requested agent will be used for prophylaxis against HAE attacks AND ALL of the following:
- The patient has a history of at least three moderate to severe acute HAE attacks per month (e.g., airway swelling, severe abdominal pain, painful facial swelling), one laryngeal attack, or is disabled more than 5 days per month by HAE AND
- The patient will NOT be using the requested agent in combination with another agent indicated for prophylaxis against HAE attacks AND
- The prescriber has agreed to reduce the quantity of the acute agent one month after authorization of the prophylactic agent by at least 2 vials or 2 syringes and will continue to assess acute agent use AND
- If Takhzyro is requested, ONE of the following:
- The patient is initiating therapy with the requested agent OR
- The patient has been treated with the requested agent for less than 6 consecutive months OR
- The patient has been treated with the requested agent for at least 6 consecutive months AND ONE of the following:
- The patient has been free of acute HAE attacks for at least 6 consecutive months and ONE of the following:
- The patient’s dose will be reduced to 300 mg every 4 weeks OR
- The prescriber has provided information in support of therapy using 300 mg every 2 weeks OR
- The patient has NOT been free of acute HAE attacks for at least 6 consecutive months AND
- Medications known to cause angioedema (i.e., ACE-Inhibitors, estrogens, angiotensin receptor blockers, dipeptidyl peptidase IV [DPP-IV] inhibitors, neprilysin inhibitors) have been evaluated and discontinued when appropriate AND
- The prescriber is a specialist in the area of the patient’s diagnosis (e.g., allergist, immunologist, hematologist, pulmonologist, medical geneticist) or the prescriber has consulted with a specialist in the area of the patient’s diagnosis AND
- The patient does NOT have any FDA labeled contraindications to the requested agent
Length of Approval: 3 months for Cinryze, 6 months for Haegarda and Orladeyo, and 9 months for Takhzyro, up to 1 month for second acute agent for HAE attacks
NOTE: For MN BPI, approve requested agent for 12 months
NOTE: If Quantity Limit applies, please refer to Quantity Limit Criteria.
*Step therapy requirement may not apply if a prior health plan paid for the medication - documentation of a paid claim may be required.
Renewal Evaluation
Target Agent(s) will be approved when ALL of the following are met:
- The patient has been previously approved for the requested agent through the plan’s Prior Authorization process AND
- The prescriber is a specialist in the area of the patient’s diagnosis (e.g., allergist, immunologist) or the prescriber has consulted with a specialist in the area of the patient’s diagnosis AND
- Information has been provided that indicates ONE of the following:
- The patient has had a decrease in the frequency of acute HAE attacks from baseline (prior to treatment) OR
- The patient has had a decrease in use of on-demand therapy AND
- The patient will NOT be using the requested agent in combination with another agent indicated for prophylaxis of HAE attacks (i.e., Cinryze, Haegarda, Orladeyo, Takhzyro) AND
- If Takhzyro is requested, ONE of the following:
- The patient has been free of acute HAE attacks for at least 6 consecutive months and ONE of the following:
- The patient’s dose will be reduced to 300 mg every 4 weeks OR
- The prescriber has provided information in support of therapy using 300 mg every 2 weeks OR
- The patient has NOT been free of acute HAE attacks for at least 6 consecutive months AND
- The patient does NOT have any FDA labeled contraindications to the requested agent
Length of Approval: 12 months
NOTE: If Quantity Limit applies, please refer to Quantity Limit Criteria.
|
QUANTITY LIMIT CLINICAL CRITERIA FOR APPROVAL
Module
|
Clinical Criteria for Approval
|
Berinert, Firazyr, icatibant, or Ruconest
|
Quantity Limit for the Target Agent(s) will be approved when ONE of the following is met:
- The requested quantity (dose) is within the program quantity limit (allows for 2 acute HAE attacks per month) OR
- The requested quantity (dose) exceeds the program quantity limit and prescriber has provided information (e.g., frequency of attacks within the past 3 months has been greater than 2 attacks per month) in support of therapy with a higher dose or quantity
Length of Approval: Initial: 6 months for first acute agent for HAE attacks, up to 1 month for second acute agent for HAE attacks; Renewal: 12 months for first acute agent for HAE attacks, up to 1 month for second acute agent for HAE attacks
|
Cinryze, Haegarda, Orladeyo, or Takhzyro
|
Quantity Limit for the Target Agent(s) will be approved when ONE of the following is met:
- The requested quantity (dose) is within the FDA labeled dose AND within the quantity limit OR
- The requested quantity (dose) exceeds the program quantity limit AND prescriber has provided information in support of therapy with a higher dose or quantity
Length of Approval: Initial: 3 months for Cinryze, 6 months for Haegarda and Orladeyo, and 9 months for Takhzyro [NOTE: For MN BPI, approve requested agent for 12 months]; Renewal: 12 months
HAEGARDA WEIGHT-BASED QUANTITY LIMITS: EXTENDED DOSING TABLE
Weight
(lb)
|
Weight (kg)
|
Quantity Limit of 3000 IU vials
per 28 days
|
Quantity Limit of 2000 IU vials
per 28 days
|
Number of
3000 IU vials used per dose
|
Number of
2000 IU vials used per dose
|
greater than 330-365
|
greater than 150-166
|
16
|
16
|
2
|
2
|
greater than 293-330
|
greater than 133-150
|
24
|
0
|
3
|
0
|
greater than 255-293
|
greater than 116-133
|
0
|
32
|
0
|
4
|
greater than 220-255
|
greater than 100-116
|
8
|
16
|
1
|
2
|
greater than 182.6-220
|
greater than 83-100
|
16
|
0
|
2
|
0
|
greater than 145-182.6
|
greater than 66-83
|
8
|
8
|
1
|
1
|
greater than 110-145
|
greater than 50-66
|
0
|
16
|
0
|
2
|
greater than or equal to 75-110
|
greater than or equal to 34-50
|
8
|
0
|
1
|
0
|
less than 75
|
less than 34
|
0
|
8
|
0
|
1
|
|
This pharmacy policy is not an authorization, certification, explanation of benefits or a contract. Eligibility and benefits are determined on a case-by-case basis according to the terms of the member’s plan in effect as of the date services are rendered. All pharmacy policies are based on (i) information in FDA approved package inserts (and black box warning, alerts, or other information disseminated by the FDA as applicable); (ii) research of current medical and pharmacy literature; and/or (iii) review of common medical practices in the treatment and diagnosis of disease as of the date hereof. Physicians and other providers are solely responsible for all aspects of medical care and treatment, including the type, quality, and levels of care and treatment.
The purpose of Blue Cross and Blue Shield of Alabama’s pharmacy policies are to provide a guide to coverage. Pharmacy policies are not intended to dictate to physicians how to practice medicine. Physicians should exercise their medical judgment in providing the care they feel is most appropriate for their patients.
Neither this policy, nor the successful adjudication of a pharmacy claim, is guarantee of payment.
ALBP _ Commercial _ CS _ Hereditary_Angioedema_PAQL _ProgSum_ 04-01-2024 _ © Copyright Prime Therapeutics LLC. January 2024 All Rights Reserved
|