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Library/Bioequivalence Trials/Players · stakeholders
chapter 08 · who runs the field

People: use cases, players, stakeholders.

Common regulatory triggers that may require a BE study · the five player categories that run the field · ten stakeholder roles. Who decides, who pays, who is liable in BE 2026.

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Use cases: what BE is actually for.

Common regulatory triggers that may require a BE study

In submission use, BE is regulated evidence work, not only research activity. It is usually triggered by specific submission pathways. The trigger determines the design (single vs multiple dose, fasted vs fed, full vs partial replicate), the reference product (RLD vs Member State innovator vs Brazilian RP), the timeline, and the inspection regime that will eventually look at the data.

21 CFR 320 + Hatch-Waxman

ANDA filing.

The original use case. US generic sponsor files Abbreviated New Drug Application against the Reference Listed Drug. Single fasted study minimum; fed study added per FDA product-specific guidance. The trigger that built the entire BE CRO industry.

EU Article 10(1)

EU generic registration.

Centralised, decentralised, mutual-recognition or national procedure. Reference product sourced from a Member State. EMA CPMP/EWP/QWP/1401/98 the canonical guidance. Member State regulator inspects the BE site directly.

351(k) BPCIA

Biosimilar PK bridging.

Comparative PK against reference biologic. Same TOST principle but executed on biologic plasma assays (LBA / hybrid LC-MS). Immunogenicity package runs in parallel.

RDC 742/2022

Brazil generic registration.

ANVISA generic or similar registration. Reference product from Brazilian list. Brazilian healthy-volunteer registry constraints. CRO inspection regime distinctive.

FDA / EMA Type II variation

Post-approval change.

Manufacturing site change, formulation modification, scale-up. SUPAC-IR / EMA variation Type II. BE bridging study against pre-change reference. Common ongoing pharma trigger across product lifecycle.

ICH M9 + FDA 2017

Biowaiver filing.

BCS Class I or III biowaiver. In vitro dissolution f2 instead of in vivo BE. Excipient effect assessment (post-M9). Most cost-effective path when BCS scope permits.

WHO PQT

WHO prequalification.

Anti-TB, anti-HIV, anti-malarial multisource generics. Reference product from WHO Comparator Product List. Annex 7 acceptance bound. LMIC public-health pathway.

CDSCO Schedule Y

India generic registration.

India-marketed innovator as reference. Schedule Y / 2018 BE Guideline. CDSCO BA-BE Centre approval. Volume of work concentrated in a narrow set of accredited Indian CROs.

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Big players: who runs the field.

CROs · generics · regulators · tech · standards

The BE ecosystem has five player categories. Generic-drug pharma sets the strategy and pays; CRO BE specialists execute most studies; regulators define the surface; tech vendors own the LIMS/EDC infrastructure; standards bodies set the harmonised guidance. Each category has a distinct centre of gravity.

CROs · BE specialists
Lambda Therapeutic Research (Ahmedabad) · Veeda Clinical Research (Ahmedabad) · Synapse Labs · Bioneeds · Sundyota Numandis · Cliantha Research. India-concentrated. Frontage Laboratories (US) · Pace Analytical · Altasciences · Celerion. North America. SGS · Quotient Sciences · BioTrial. Europe. Trial conduct · volunteer recruitment · bioanalysis · CSR ownership.
Generic-drug pharma · sponsors
Teva · Sandoz · Mylan / Viatris · Sun Pharma · Cipla · Aurobindo · Lupin · Dr Reddy's · Zydus Lifesciences · Hetero · Glenmark · Torrent. Sponsors driving ANDA + EU generic + Brazil + WHO PQ programmes. India-concentrated supply side. Hikma · Apotex · Sandoz Hexal for European/North American generic strategy.
Innovator pharma · biosimilar / lifecycle
Pfizer (Hospira biosimilar portfolio) · Sandoz · Amgen · Samsung Bioepis · Celltrion · Biocon. Biosimilar PK bridging studies. Innovators also run BE for post-approval Type II variations across their lifecycle portfolios.
Regulators
FDA OGD (Office of Generic Drugs · ANDA review) · FDA OSIS (Office of Study Integrity and Surveillance · BE inspections) · EMA CHMP + national authorities (BfArM, AIFA, ANSM, MHRA pre-Brexit) · ANVISA Gerência de Medicamentos Genéricos · WHO PQT Prequalification Team · CDSCO + Subject Expert Committee · PMDA (Japan).
Tech vendors · LIMS / EDC / stats
Veeva Vault EDC · Medidata Rave · Oracle Inform. Clinical EDC. Watson LIMS (Thermo Fisher) · SCIEX OS · Waters MassLynx + iSubmit. Bioanalytical LIMS. SAS · Phoenix WinNonlin (Certara) · R / ncar / nlmixr. Statistics + PK calculation. Veeva CTMS for trial conduct oversight.
Standards bodies & academia
ICH (M9 BCS biowaivers · M13A IR oral BE · M13B/C in development) · AAPS · EUFEPS Bioequivalence Section · FIP. Academic centres: U Maryland CERSI · U North Carolina Eshelman School · Uppsala University Pharmacometrics · Manipal · Jamia Hamdard (BE methodology). Crystal City conference series · ICH expert working groups.
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Stakeholders: interests & leverage.

Who decides · who pays · who is affected

Each stakeholder in a BE programme has a distinct interest and a distinct lever. Reading the operating context means knowing who responds when the study is challenged — whether by a regulatory question, inspection observation, site finding, or volunteer adverse event. Ten roles cover the field.

Generic-drug sponsor
Interestshortest possible time-to-ANDA-approval · lowest BE study cost
LeverageCRO selection · pathway selection (FDA vs WHO PQ vs ANVISA creates different BE expense and timeline)
Innovator pharma · biosimilar
Interestregulatory acceptance of comparative PK without repeating Phase 3 efficacy
Leverageanalytical similarity package depth · immunogenicity assay strategy
CRO · BE specialist
Intereststudy throughput · inspection readiness · healthy-volunteer pool retention
LeverageCPU bed capacity · bioanalytical lab queue time · LC-MS/MS skill scarcity
Healthy volunteer
Interestsafety during dosing · honoraria payment · eligibility for next study after washout
Leverageindirect (registry compliance · informed consent withdrawal)
Clinical investigator · CPU PI
Interestsafety data integrity · protocol compliance · site reputation across sponsors
Leverageprotocol compliance authority · SAE reporting · biospecimen chain-of-custody
Regulator · FDA OGD
Intereststatistical validity of TOST · reference-product chain-of-custody · ISR compliance
Leveragedeficiency letters · refuse-to-receive · ANDA approvability decisions · CR letters
Regulator · FDA OSIS
InterestBE site data integrity · healthy-volunteer protection · bioanalytical raw-data audit
Leverage483 observations · warning letters · inspection observations · warning letters · data-reliability findings
Regulator · EMA + Member States
Interestreference Member State sourcing chain · statistical validity · cross-Member-State variability
Leveragemajor objection authority · national procedure withholding · Member-State-level inspection
Regulator · ANVISA
InterestBrazilian RP sourcing · volunteer registry compliance · BE CRO certification
LeverageBrazil-specific regulatory expectations · CRO/site compliance findings · product-specific evidence questions
Payer · health system
Interestgeneric substitutability · cost-effectiveness · AB-rated equivalents
Leverageformulary inclusion · reimbursement decisions · national pricing controls
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Official source register.

Regulator / ICH anchors
ICH / FDA

ICH M13A bioequivalence guideline.

Official FDA-hosted page for ICH M13A on bioequivalence for immediate-release solid oral dosage forms. Use as the first harmonised anchor for conventional oral IR BE framing.

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ICH M9

BCS-based biowaiver guidance.

Official ICH M9 Step 4 guideline. Use for BCS classification, solubility/permeability thinking, and eligible biowaiver conditions.

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ICH M10

Bioanalytical method validation and study sample analysis.

Official ICH M10 Step 4 guideline. Use for the bioanalytical evidence layer that supports BA/BE concentration data.

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FDA PSG

Product-specific guidances for generic development.

FDA product-specific guidance collection. Use before protocol lock because product-level recommendations can change design, fed/fasted, analyte, and BE expectations.

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21 CFR 320

US bioavailability and bioequivalence regulation.

Electronic Code of Federal Regulations anchor for US BA/BE definitions and requirements. Use for statutory/regulatory context, not as a complete study-design manual.

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EMA

Guideline on the investigation of bioequivalence.

EMA scientific guideline landing page for BE investigation. Use for EU framing, while checking product-specific or updated procedural context where relevant.

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WHO

Multisource generic products and interchangeability.

WHO IRIS record for multisource pharmaceutical product guidance. Use as a WHO anchor for generic interchangeability and BE expectations in broader access settings.

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