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Interstitial Lung Disease (ILD) Prior Authorization with Quantity Limit Program Summary

Policy Number: PH-1124

 

This prior authorization applies to Blue Partner, Commercial, NetResults A series, SourceRx and Health Insurance Marketplace formularies.

POLICY REVIEW CYCLE                                                                                                                                                                           

Effective Date

Date of Origin 

10/1/2023              

FDA APPROVED INDICATIONS AND DOSAGE

Agent(s)

FDA Indication(s)

Notes

Ref#

Esbriet®

(pirfenidone)*

Tablet

Capsule

Treatment of idiopathic pulmonary fibrosis (IPF)

*- generic available

1

Ofev®

(nintedanib)

Capsule

Treatment of idiopathic pulmonary fibrosis (IPF)

Slow the rate of decline in pulmonary function in patients with systemic sclerosis-associated interstitial lung disease (SSc-ILD)

Treatment of chronic fibrosing interstitial lung diseases (ILDs) with a progressive phenotype

2

See package insert for FDA prescribing information:  https://dailymed.nlm.nih.gov/dailymed/index.cfm

CLINICAL RATIONALE

Interstitial Lung Disease

Interstitial lung diseases (ILD) encompass a varied group of more than 200 lung disorders that affect the tissue and space around the alveoli. They are classified together because of similar physiologic, radiographic, clinical, or pathologic manifestations: respiratory symptoms such as shortness of breath and cough, specific chest radiographic abnormalities, typical changes on pulmonary function tests in which lung volume is decreased, and characteristic microscopic patterns of inflammation and fibrosis. Fibrosis is characterized by an increased amount and abnormal structure of the connective tissue, with lung biopsies with a predominance of fibrosis typically indicating advanced disease and poor prognosis.(11)

The underlying causes of ILD can be classified into four categories: diseases associated with a condition that affects other parts of the body (e.g., autoimmune, collagen vascular disease), exposure to agents known to damage the lungs (e.g., medications, occupational exposures [e.g., asbestos, tobacco smoke]), genetic abnormalities (e.g., Hermansky-Pudlak syndrome), or idiopathic etiology (the most common form).(13)

Idiopathic Pulmonary Fibrosis (IPF)

Idiopathic pulmonary fibrosis (IPF) is a form of chronic, progressive fibrosing interstitial pneumonia of unknown origin occurring primarily in older adults and is limited to the lungs.(5,6) IPF is associated with the histopathologic and/or radiologic pattern of usual interstitial pneumonia (UIP).(4,6,17) IPF is characterized by fibroblast foci, featuring vigorous replication of mesenchymal cells and disposition of extracellular matrix. It is thought that repeated episodes of acute lung injury, due to unknown stimulus, leads to wound healing and fibrosis, with loss of lung function.(7) The natural progression can vary with some patients remaining stable for extended periods of time; some having steady, but rapid progression; and some patients experiencing acute exacerbations.(3) Historically, a diagnosis of IPF has been associated with a poor prognosis with many only living for 3-5 years post diagnosis. The estimated prevalence of IPF within the United States has been difficult to establish due to the historical lack of a uniform definition, evolving diagnostic criteria, and difference in case-finding methodologies and study designs. The range is between 14-63 per 100,000 population with an annual incidence of approximately 7-16 per 100,000 population.(4)

Guidelines suggest that IPF be considered in adult patients presenting with unexplained chronic exertional dyspnea, cough, bibasilar inspiratory crackles, and/or finger clubbing.(4,6)

An accurate diagnosis of IPF is a difficult and challenging process. The accuracy of the diagnosis increases with an integrated multidisciplinary approach. This includes dynamic discussion between pulmonologists, radiologists, and pathologists (when appropriate) who are experienced in the diagnosis of ILD.(3) The diagnosis of IPF requires exclusion of other known causes of ILD (e.g., domestic and occupational environmental exposures, connective tissue disease, and drug toxicity), and either the presence of a UIP pattern on HRCT in patients not subjected to surgical lung biopsy (SLB) OR specific combinations of HRCT patterns and histopathological patterns in patients subjected to SLB.(3,6,17)

The 2018 and updated 2022 guidelines provide a new diagnostic algorithm and schema for correlating histologic and radiologic findings in patients with suspected IPF.(6,17) Aspects of this algorithm include criteria for four diagnostic categories for patterns of UIP based on HRCT findings (i.e., UIP, probable UIP, indeterminate for UIP, and alternative diagnosis), and four levels of certainty for histopathologic diagnosis (i.e., UIP, probable UIP, indeterminate for UIP, and alternative diagnosis).

UIP is characterized on HRCT by the presence of peripheral, basilar-predominant opacities associated with honeycombing and traction bronchiectasis-bronchiolectasis. In patients whose HRCT does not demonstrate a UIP pattern, the surgical lung biopsy may demonstrate UIP pattern on histopathology.(6,17) Table 1 below shows the algorithm for diagnosis with the updated guidelines.

Table 1. Idiopathic pulmonary fibrosis diagnosis based upon HRCT and biopsy patterns(6,17)

IPF Suspectedc

Histopathology Pattern

UIP

Probable UIP

Indeterminate for UIP (or biopsy not performed)

Alternative Diagnosis

 

 

HRCT Pattern

UIP

IPF

IPF

IPF

Non-IPF diagnosis

Probable UIP

IPF

IPF

IPF (likely)d

Non-IPF diagnosis

Indeterminate

IPF

IPF (likely)d

Indeterminatef

Non-IPF diagnosis

Alternative Diagnosis

IPF (likely)d

Indeterminatef

Non-IPF diagnosis

Non-IPF diagnosis

c - ”Clinically suspected of having IPF” = unexplained patterns of bilateral pulmonary fibrosis on a chest radiography or chest CT, bibasilar inspiratory crackles, and age greater than 60 years. (Middle aged adults [greater than 40 years and less than 60 years], can rarely present with otherwise clinical features, especially in patients with features suggesting familial pulmonary fibrosis.)

d - IPF is the likely diagnosis when any of the following features are present:

  • Moderate-to-severe traction bronchiectasis and/or bronchiolectasis (defined as mild traction bronchiectasis and/or bronchiolectasis in four or more lobes, including the lingula as a lobe, or moderate to severe traction bronchiectasis in two or more lobes) in a man over age 50 years or in a woman over age 60 years
  • Extensive (greater than 30%) reticulation on HRCT and an age greater than 70 years
  • Increased neutrophils and/or absence of lymphocytosis in BAL fluid
  • Multidisciplinary discussion reaches a confident diagnosis of IPF

f - Indeterminate for IPF

  • Without an adequate biopsy remains indeterminate
  • With an adequate biopsy may be reclassified to a more specific diagnosis after multidisciplinary discussion and/or additional consultation

Prior to the simultaneous approvals of Esbriet (pirfenidone) and Ofev (nintedanib), there was no FDA approved pharmacologic therapy for idiopathic pulmonary fibrosis. The updated ATS/ERS/JRS/ALAT (American Thoracic Society, European Respiratory Society, Japanese Respiratory Society, and Latin American Thoracic Society) clinical practice guidelines address nintedanib and pirfenidone treatment for IPF. The guidelines suggest that clinicians use nintedanib or pirfenidone in patients with IPF (conditional recommendation, moderate confidence in estimates of effects). As with other interventions, the available evidence focuses on patients with IPF with mild to moderate impairment in pulmonary function tests; it is unknown whether the therapeutic benefits would differ in patients with a more severe impairment in pulmonary function testing or those with other comorbidities. The evidence does not allow suggestions about the optimal duration of therapy, and it is unknown how long the treatment effect endures with ongoing drug therapy.(5,17) 

Currently, there are no head-to-head trials comparing the two agents. A retrospective cohort study assessed the clinical effectiveness of nintedanib and pirfenidone in the treatment of IPF. The primary outcome was all-cause mortality, which was seen reduced in the treated cohort versus the untreated cohort. This mortality benefit was only observed for the first two years of follow-up. No significant differences were noted in all-cause mortality between patients treated with nintedanib versus pirfenidone; however, pirfenidone had a slightly more favorable trend.(14)

The possibility that combined therapy might be of greater benefit is under investigation, with results supporting further research into combination treatment with pirfenidone and nintedanib. An open-label, randomized trial (INJOURNEY) evaluating the safety and tolerability of nintedanib with add-on pirfenidone demonstrated a manageable safety and tolerability profile in patients with IPF, in line with the adverse event profiles of each drug.(15) Another trial, open-label, 24-week, single-arm, phase IV study, assessed safety and tolerability of treatment with pirfenidone and nintedanib in patients with IPF. Combined pirfenidone and nintedanib use for 24 weeks was tolerated by the majority of patients with IPF and associated with a similar pattern of adverse events expected for either treatment alone.(16)

Systemic Sclerosis (Scleroderma)-Associated Interstitial Lung Disease (ILD)

Systemic sclerosis is a connective tissue disease (CTD) that affects numerous organ systems, including skin, blood vessels, heart, lungs, kidneys, gastrointestinal, and musculoskeletal. Pulmonary disease is the leading cause of death in patients with systemic sclerosis, and ILD is a common manifestation that tends to occur early in the course of systemic sclerosis(8)

The American College of Rheumatology (ACR) and European League Against Rheumatism (EULAR) collaborated on classification criteria for the diagnosis of systemic sclerosis, in which they note that systemic sclerosis-associated ILD is diagnosed when there is radiographic evidence of diffuse parenchymal lung disease in patients with systemic sclerosis. The ACR/EULAR criteria note that ILD is defined as pulmonary fibrosis seen on HRCT or chest radiography, most pronounced in the basilar portions of the lungs.(10)

The American College of Rheumatology (ACR) published a treatment algorithm for systemic sclerosis and related conditions. The ACR recommends the following treatment options for ILD associated with systemic sclerosis:(9)

Induction therapy:

  • Mycophenolate mofetil (MMF) as first line therapy
  • IV cyclophosphamide as second line therapy
  • Rituximab as third line therapy
  • Lung transplant or hemopoietic stem cell transplant for select patients as fourth line therapy 

Maintenance therapy:

  • Mycophenolate mofetil (MMF) as first line therapy
  • Azathioprine as second line therapy
  • IV or oral cyclophosphamide as third line therapy

Chronic Fibrosing Interstitial Lung Disease with Progressive Phenotype

Patients that have a progressive fibrosing phenotype tend to be characterized by an increasing extent of fibrosis on HRCT, decreasing lung function, worsening of symptoms and quality of life, and early death despite treatment. The progressive phenotype is similar to IPF in clinical behavior and in many of the underlying pathogenic mechanisms, such as repeated chronic epithelial or vascular injuries leading to cell destruction and unregulated repair, that drive a self-sustaining process of pulmonary fibrosis.(12) There are currently no guidelines to define the management of patients with ILD with a progressive phenotype.(11)

Efficacy(2)

The clinical efficacy of Ofev has been studied in patients with chronic fibrosing ILDs with a progressive phenotype in a randomized, double-blind, placebo-controlled phase 3 trial (Study 5 [NCT02999178]). A total of 663 patients were randomized in a 1:1 ratio to receive either Ofev 150 mg twice daily or matching placebo for at least 52 weeks. Randomization was stratified based on high resolution computed tomography (HRCT) fibrotic pattern as assessed by central readers. The primary endpoint was the annual rate of decline in FVC (in mL) over 52 weeks. Other endpoints included time to first acute ILD exacerbation and time to death. 

Patients with a clinical diagnosis of a chronic fibrosing ILD were selected if they had relevant fibrosis (greater than 10% fibrotic features) on HRCT and presented with clinical signs of progression (defined as FVC decline greater than or equal to 10%, FVC decline greater than or equal to 5% and less than 10% with worsening symptoms or imaging, or worsening symptoms and worsening imaging all in the 24 months prior to screening). Patients were required to have an FVC greater than or equal to 45% of predicted and a diffusion capacity of the lungs for carbon monoxide (DLCO) 30% to less than 80% of predicted. Patients were required to have progressed despite management deemed appropriate in clinical practice by investigators for the patient’s relevant ILD. 

Patients with IPF, relevant airways obstruction (i.e., pre-bronchodilator FEV1/FVC less than 0.7), or significant pulmonary hypertension were excluded from the trial. Patients with greater than 1.5 times ULN of ALT, AST, or bilirubin, patients with a known risk or predisposition to bleeding, patients receiving a full dose of anticoagulation treatment, and patients with a recent history of myocardial infarction or stroke were excluded.

The underlying clinical ILD diagnoses in groups represented in the trial were hypersensitivity pneumonitis (26%), autoimmune ILDs (26%), idiopathic nonspecific interstitial pneumonia (19%), unclassifiable idiopathic interstitial pneumonia (17%), and other ILDs (12%).

There was a statistically significant reduction in the annual rate of decline in FVC (in mL) over 52 weeks in patients receiving Ofev compared to patients receiving placebo. The annual rate of decline in FVC (in mL) over 52 weeks was significantly reduced by 107 mL in patients receiving Ofev compared to patients receiving placebo. For the majority of patients, the decline in lung function was less on Ofev than on placebo. The risk of first acute ILD exacerbation did not show a statistically significant difference between the Ofev group compared to placebo (52-week treatment period: HR 0.72, [95% CI: 0.38, 1.37]; whole trial: HR 0.63 [95% CI: 0.37, 1.07]). Survival was evaluated for Ofev compared to placebo in Study 5 to support the primary endpoint (FVC). All-cause mortality was assessed over the study duration and available follow-up period, irrespective of cause of death and whether patients continued treatment. All-cause mortality did not show a statistically significant difference (52-week treatment period: HR 0.94 [95% CI: 0.47, 1.86]; whole trial: HR 0.78 [95% CI: 0.50, 1.21]).

Safety

Neither Esbriet nor Ofev have any FDA labeled contraindications.(1,2)

REFERENCES                                                                                                                                                                            

Number

Reference

1

Esbriet prescribing information. Laurus Labs Limited. April 2022.

2

Ofev prescribing information. Boehringer Ingelheim Pharmaceuticals, Inc. January 2022.

3

An Official American Thoracic Society/European Respiratory Society Statement: Update of the International Multidisciplinary Classification of the Idiopathic Interstitial Pneumonias. Am J Respir Crit Care Med. 2013;188(6):733–748.

4

Nalysnyk L, Cid-Ruzafa J, Rotella P, Esser D. Incidence and Prevalence of Idiopathic Pulmonary Fibrosis: Review of the Literature. Eur Respir Rev. 2012;21(126):355-361.

5

An Official ATS/ERS/JRS/ALAT Clinical Practice Guideline: Treatment of Idiopathic Pulmonary Fibrosis - An Update of the 2011 Clinical Practice Guideline. Am J Resp Crit Care. 2015;192(2):e3-e19.

6

Diagnosis of Idiopathic Pulmonary Fibrosis: An Official ATS/ERS/JRS/ALAT Clinical Practice Guideline. Am J Respir Crit Care Med. 2018 Sep;198(5):e44-e68.

7

Raghu G, Montesi S, et al. Pathogenesis of Idiopathic Pulmonary Fibrosis. UpToDate. Literature review current through September 2022. Last updated August 2022.

8

Update of EULAR Recommendations for the Treatment of Systemic Sclerosis. Ann Rheum Dis. 2017;76:1327-1339.

9

Fernández‐Codina A, Walker KM, Pope JE. Treatment Algorithms for Systemic Sclerosis According to Experts. Arthritis Rheum. 2018 Nov;70(11):1820-1828.

10

van den Hoogen F, Khanna D, Fransen J, et al. Classification Criteria for Systemic Sclerosis: An American College of Rheumatology/European League Against Rheumatism Collaborative Initiative. Arthritis Rheum. 2013 Nov;65(11):2737–2747.

11

Cottin V, Wollin L, Fischer A, et al. Fibrosing Interstitial Lung Diseases: Knowns and Unknowns. Eur Respir Rev. 2019;28:1-9.

12

Kolb M, Vašáková M. The Natural History of Progressive Fibrosing Interstitial Lung Diseases. Respir Res. 2019;20(57):1-8.

13

Cool CD, et al. Idiopathic Interstitial Pneumonias: Classification and Pathology. UpToDate. Literature review current through September 2022. Last updated February 2021.

14

Dempsey TM, Sangaralingham LR, Yao X, et al. Clinical Effectiveness of Antifibrotic Medications for Idiopathic Pulmonary Fibrosis. Am J Respir Crit Care Med. 2019;200(2):168-174.

15

Vancheri C, Kreuter M, Richeldi L, et al. Nintedanib with Add-on Pirfenidone in Idiopathic Pulmonary Fibrosis: Results of the INJOURNEY Trial. Am J Respir Crit Care Med. 2018;197(3):356-363.

16

Flaherty KR, Fell CD, Huggins JT, et al. Safety of Nintedanib Added to Pirfenidone Treatment for Idiopathic Pulmonary Fibrosis. Eur Respir J. 2018;52(2):1-10.

17

Idiopathic Pulmonary Fibrosis (an Update) and Progressive Pulmonary Fibrosis in Adults: An Official ATS/ERS/JRS/ALAT Clinical Practice Guideline. 2022;205(9):e18.

 

POLICY AGENT SUMMARY PRIOR AUTHORIZATION

Target Brand Agent(s)

Target Generic Agent(s)

Strength

Targeted MSC

Available MSC

Final Age Limit

Preferred Status

Ofev

nintedanib esylate cap

100 MG ; 150 MG

M ; N ; O ; Y

N

Esbriet

pirfenidone cap  ; pirfenidone tab

267 MG ; 534 MG ; 801 MG

M ; N ; O ; Y

N ; O ; Y

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

Pirfenidone Tab 534MG

534 MG

21

Tablets

180

DAYS

Esbriet

Pirfenidone Cap 267 MG

267 MG

180

Capsules

30

DAYS

Esbriet

Pirfenidone Tab 267 MG

267 MG

180

Tablets

30

DAYS

Esbriet

Pirfenidone Tab 801 MG

801 MG

90

Tablets

30

DAYS

Ofev

nintedanib esylate cap

100 MG ; 150 MG

60

Capsules

30

DAYS

CLIENT SUMMARY – PRIOR AUTHORIZATION

Target Brand Agent Name(s)

Target Generic Agent Name(s)

Strength

Client Formulary

Esbriet

pirfenidone cap  ; pirfenidone tab

267 MG ; 534 MG ; 801 MG

Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx

Ofev

nintedanib esylate cap

100 MG ; 150 MG

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

Pirfenidone Tab 534MG

534 MG

Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx

Esbriet

Pirfenidone Cap 267 MG

267 MG

Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx

Esbriet

Pirfenidone Tab 267 MG

267 MG

Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx

Esbriet

Pirfenidone Tab 801 MG

801 MG

Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx

Ofev

nintedanib esylate cap

100 MG ; 150 MG

Blue Partner ; Commercial ; GenPlus ; Health Insurance Marketplace ; NetResults A Series ; SourceRx

PRIOR AUTHORIZATION CLINICAL CRITERIA FOR APPROVAL

Module

Clinical Criteria for Approval

Initial Evaluation
Target Agent(s) will be approved when ALL of the following are met:

  1. ONE of the following:
    1. The patient has a diagnosis of idiopathic pulmonary fibrosis (IPF) AND ALL of the following:
      1. Other known causes of interstitial lung disease (ILD) have been excluded (e.g., domestic and occupational environmental exposures, connective tissue diseases, drug toxicities, alternative diagnoses, etc) AND
      2. ONE of the following:
        1. The patient had a high-resolution computed tomography (HRCT) scan with results showing a pattern for usual interstitial pneumonia (UIP) OR
        2. The patient had a surgical lung biopsy with pathology confirming UIP OR
        3. The patient had a HRCT scan with results showing a pattern for probable UIP AND a surgical lung biopsy with pathology indicating probable UIP OR
    2. The patient has a diagnosis of systemic sclerosis-associated interstitial lung disease (SSc-ILD) AND ALL of the following:
      1. The requested agent is Ofev AND
      2. The patient’s diagnosis has been confirmed on high-resolution computed tomography (HRCT) or chest radiography scans AND
      3. ONE of the following:
        1. The patient has tried and had an inadequate response to ONE conventional agent (i.e., mycophenolate mofetil, cyclophosphamide, azathioprine) OR
        2. The patient has an intolerance or hypersensitivity to ONE conventional agent OR
        3. The patient has an FDA labeled contraindication to ALL conventional agents OR
    3. The patient has a diagnosis of chronic fibrosing interstitial lung disease (ILD) with a progressive phenotype AND ALL of the following:
      1. The requested agent is Ofev AND
      2. The patient has greater than 10% fibrotic features on HRCT AND
      3. The patient presented with clinical signs of progression, defined by at least ONE of the following:
        1. FVC decline greater than or equal to 10% OR
        2. FVC decline greater than or equal to 5% and less than 10% with worsening symptoms or imaging OR
        3. Worsening symptoms and worsening imaging within the past 24 months AND
      4. The patient has an FVC greater than or equal to 45% of predicted AND
      5. The patient has a diffusion capacity of the lungs for carbon monoxide (DLCO) between 30% to less than 80% of predicted AND
      6. The patient does NOT meet any of the following:
        1. A diagnosis of IPF
        2. Relevant airway obstructions (i.e., pre-bronchodilator FEV1/FVC less than 0.7)
        3. Significant pulmonary hypertension
        4. Greater than 1.5 times the upper limit of normal for ALT, AST, or bilirubin
        5. Known risk or predisposition to bleeding
        6. Receiving full dose anticoagulation treatment
        7. Recent history of MI or stroke OR
    4. The patient has another FDA approved indication for the requested agent AND
  2. The prescriber is a specialist in the area of the patient's diagnosis (e.g., pathologist, pulmonologist, radiologist, rheumatologist) or the prescriber has consulted with a specialist in the area of the patient's diagnosis AND
  3. The patient will NOT be using the requested agent in combination with another agent included in this prior authorization program AND
  4. 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.

 

Renewal Evaluation
Target Agent(s) will be approved when ALL of the following are met:

  1. The patient has been previously approved for the requested agent through the plan’s Prior Authorization process AND
  2. The patient has had clinical benefit with the requested agent AND
  3. The prescriber is a specialist in the area of the patient’s diagnosis (e.g., pathologist, pulmonologist, radiologist, rheumatologist) or the prescriber has consulted with a specialist in the area of the patient’s diagnosis AND
  4. The patient will NOT be using the requested agent in combination with another agent included in this prior authorization program AND
  5. 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

Quantity Limit for the Target Agent(s) will be approved when ONE of the following is met:

  1. The requested quantity (dose) does NOT exceed the program quantity limit OR
  2. ALL of the following:
    1. The requested quantity (dose) is greater than the program quantity limit AND
    2. The requested quantity (dose) does NOT exceed the maximum FDA labeled dose for the requested indication AND
    3. The requested quantity (dose) cannot be achieved with a lower quantity of a higher strength that does not exceed the program quantity limit OR
  3. ALL of the following:
    1. The requested quantity (dose) is greater than the program quantity limit AND
    2. The requested quantity (dose) is greater than the maximum FDA labeled dose for the requested indication AND
    3. The prescriber has provided information in support of therapy with a higher dose for the requested indication

Length of Approval:  12 months

 

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.

 

 

Commercial _ PS _ Interstitial Lung Disease (ILD) Prior Authorization with Quantity Limit _ProgSum_ 10/1/2023