Development pathways for subcutaneous formulations of biologics versus biosimilar development

Zharkov, Artem; Barton, Bettina; Heinzmann, Dominik; Bakalos, Georgios; Schreitmüller, Thomas

doi:10.1080/23808993.2019.1585806

Cited by 6 publications

(8 citation statements)

References 34 publications

(45 reference statements)

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“…Pharmacovigilance, the practice of identifying adverse events during routine clinical use of a drug, is essential to ensuring patient safety [74,75]. It is needed not only to identify events too rare to be observed in the randomized controlled setting, but also to identify issues related to a particular batch or lot of a product (i.e., manufacturing-or storage-related issues).…”

Section: Traceability Of Biologic Productsmentioning

confidence: 99%

“…Because these changes can introduce product variability, the sponsor of an agent undergoing manufacturing changes undertakes comparability assessments throughout the manufacturing process, including product intermediates, ensuring that any variability introduced by manufacturing changes falls within pre-specified limits. Since the molecule generated before and after the manufacturing change is produced by the same sponsor in the same cell line [75], with impurities, inactive ingredients, and microheterogeneity (Table 1) kept within regulatoryapproved specifications, and since any manufacturing change must be approved by health authorities, the consistency of the biologic product is maintained over time. In contrast, biosimilarity exercises for a biosimilar can occur only with the commercially available version of the innovator (i.e., the final product) [12], not with intermediates (as would occur in a singlesupply chain).…”

Section: Manufacturingmentioning

confidence: 99%

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The Automatic Substitution of Biosimilars: Definitions of Interchangeability are not Interchangeable

et al. 2021

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In the USA, an interchangeability designation provides biosimilar sponsors with a pathway for achieving what is standard for small-molecule generics: pharmacy-level auto-substitution for an innovator. No other major health authority links interchangeability to automatic substitution, as all require the involvement of the prescriber or patient in a medication change. This editorial considers the clinical impact and practicality of auto-substitution. First, interchangeability is linked to non-medical switching (NMS), the practice of switching treatment in patients with stable disease for non-clinical reasons. NMS may generate negative sentiment in those unwilling or reluctant to switch, which can adversely impact treatment outcomes (i.e., nocebo effect). Indeed, in real-world studies of tumor necrosis factor inhibitors, discontinuation rates have been shown to be higher in patients switched to biosimilars for non-medical reasons than in historical cohorts maintained on innovators. Second, interchangeability may impede pharmacovigilance and traceability, as not all jurisdictions require innovators and biosimilars to have distinct biologic names. Third, an interchangeability designation from the US Food and Drug Administration only permits a biosimilar to be automatically substituted for its innovator, not other biosimilars (if available). Pharmacist education would be needed to avoid off-label, automatic substitution among biosimilars of a single innovator. Last, once granted, an interchangeability designation exists in perpetuity under current US federal law. However, the supply chains of innovators and biosimilars are maintained independently, with no requirement for reconfirmation of biosimilarity or interchangeability. We feel that additional guidance is needed for the auto-substitution of biosimilars and innovators to become a reality.

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Section: Traceability Of Biologic Productsmentioning

confidence: 99%

Section: Manufacturingmentioning

confidence: 99%

The Automatic Substitution of Biosimilars: Definitions of Interchangeability are not Interchangeable

et al. 2021

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“…as those programs offered by the originator product [ 80 ]. Switching patients once or multiple times between therapies can also lead to concerns related to product delivery devices and injection-site reactions because the biosimilar may not use the same delivery device, formulation, dosage, or dosing interval as the originator [ 81 – 84 ]. Differences in formulation may also influence patient satisfaction and adherence [ 81 ].…”

Section: Challenges With Multiple Switchingmentioning

confidence: 99%

The Challenges of Switching Therapies in an Evolving Multiple Biosimilars Landscape: A Narrative Review of Current Evidence

Feagan

Marabani

et al. 2020

Adv Ther

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With the increasing availability of biosimilars, the practice of switching therapies for non-medical reasons between an originator biologic and an analogous biosimilar has become more common. The evidence to support this practice mostly comes from single-switch randomized controlled trials (RCTs) and real-world (RW) evidence studies. However, as more biosimilars of the same originator enter the market, multiple switching events between originators and biosimilars is becoming a reality, despite limited evidence to support the efficacy and safety of such practice. Some countries have established guidelines, policies, or laws related to interchangeability and/or automatic substitution, whereas others have left these practices unregulated or controlled by other components of the healthcare system. Collectively, guidelines on single non-medical switching are often vague, with even less focus given to multiple non-medical switching, leaving this practice mostly unregulated. This narrative review will first discuss the current regulatory perspectives on non-medical switching and challenges associated with switching therapies, particularly with the availability of multiple biosimilars. We will then review the current evidence from RCTs and RW studies in the light of three different multiple-switch scenarios currently taking place in clinical practice: switching between an originator and a single biosimilar, switching between biosimilars of the same originator, and the clinical practice of switching back to the originator (i.e., switchbacks) after a failure of the initial non-medical switch to the analogous biosimilar.

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“…Unlike small molecule drugs, administering effective doses of mAbs orally can be extremely challenging due to their physical instability, low permeability across the gastrointestinal membrane, and vulnerability to enzymatic activity. 5 , 6 Most biologic products have traditionally been formulated at low concentrations (<30 mg/mL) convenient for IV infusion to maximize biologic stability, 7 , 8 lower manufacturing costs during development by decreasing the amount of drug needed for the stability program, and reduce waste during clinical dose-escalation studies. Altogether, compared to high-concentration formulations, low-concentration biologic drug formulations are easier and less costly to develop and are more stable due to their lower concentrations.…”

Section: Introductionmentioning

confidence: 99%

Monoclonal antibody and protein therapeutic formulations for subcutaneous delivery: high-concentration, low-volume vs. low-concentration, high-volume

Desai,

Kundu,

Hageman

et al. 2023

mAbs

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Biologic drugs are used to treat a variety of cancers and chronic diseases. While most of these treatments are administered intravenously by trained healthcare professionals, a noticeable trend has emerged favoring subcutaneous (SC) administration. SC administration of biologics poses several challenges. Biologic drugs often require higher doses for optimal efficacy, surpassing the low volume capacity of traditional SC delivery methods like autoinjectors. Consequently, high concentrations of active ingredients are needed, creating time-consuming formulation obstacles. Alternatives to traditional SC delivery systems are therefore needed to support higher-volume biologic formulations and to reduce development time and other risks associated with high-concentration biologic formulations. Here, we outline key considerations for SC biologic drug formulations and delivery and explore a paradigm shift: the flexibility afforded by low-to-moderate-concentration drugs in high-volume formulations as an alternative to the traditionally difficult approach of high-concentration, low-volume SC formulation delivery.

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Development pathways for subcutaneous formulations of biologics versus biosimilar development

Cited by 6 publications

References 34 publications

The Automatic Substitution of Biosimilars: Definitions of Interchangeability are not Interchangeable

The Automatic Substitution of Biosimilars: Definitions of Interchangeability are not Interchangeable

The Challenges of Switching Therapies in an Evolving Multiple Biosimilars Landscape: A Narrative Review of Current Evidence

Monoclonal antibody and protein therapeutic formulations for subcutaneous delivery: high-concentration, low-volume vs. low-concentration, high-volume

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