Pipeline & Programs

An advancing, focused development pipeline.

Three programs targeting distinct indications where gut dysbiosis drives disease and existing therapies fall short. Each anchored in the same defined-consortium platform.

Pipeline Overview

A staged development program

Three programs across distinct indications where gut dysbiosis drives disease. Filter by therapeutic area, or open any program for mechanism, status, and trial detail.

Therapeutic area

Phase

3 programs

ModalityDefined consortium — purified, clonally-banked Clostridia

Current stageIND-enabling — Phase 1-ready

Next milestoneIND / CTA submission → first-in-human (planned)

Clinical trialRESTORe-101 · Phase 1 (planned) — registered at IND

Mechanism

Antibiotics that clear C. difficile also collapse the gut's secondary-bile-acid and short-chain-fatty-acid metabolism — the very functions that keep the pathogen suppressed — leaving patients vulnerable to recurrence.⁵ GR-101 is a defined consortium of purified, clonally-banked Clostridia selected to reconstitute those functions: producing secondary bile acids that block C. difficile spore germination and outgrowth, and competing for the nutrients it needs to bloom.⁴

This is the modality and indication already validated by the first generation of defined and standardised consortia — VE303 (8 strains) cut recurrence odds by more than 80% in Phase 2, and SER-109 (VOWST) is FDA-approved — placing GR-101 on well-precedented ground.^1,2 RESTORe-101, our planned Phase 1, is a randomised, double-blind, placebo-controlled study of safety, tolerability, and strain engraftment, with longitudinal bile-acid and SCFA sampling as the mechanistic readout.

Consortium composition

Representative functional classes of the GR-101 consortium. Exact isolates, ratios, and cell-bank identifiers are held as trade secret; the classes shown are anchored to published mechanism.

Strain class	Functional role	Evidence
GRC-101·01	Clostridium scindens-class — 7α-dehydroxylating	Secondary bile acids (DCA/LCA) block C. difficile germination [4]
GRC-101·02	Clostridium hiranonis-class	Bile-acid 7α-dehydroxylation capacity [4]
GRC-101·03	Blautia producta-class	Nutrient competition & colonisation resistance [5]
GRC-101·04	Clostridium cluster IV — butyrogenic	SCFA restoration after antibiotic depletion [13]
GRC-101·05	Commensal Clostridia (cluster XIVa)	Network restoration & engraftment [2]

ModalityImmune-modulating consortium

Current stagePreclinical — IND preparation

Next milestoneIND filing · first-in-human 2027

Clinical trialNot yet registered

Mechanism

GR-201 pairs butyrate-producing commensals with Treg-inducing Clostridia to rebuild two collapsed functions of the ulcerative-colitis gut at once: short-chain-fatty-acid output and mucosal immune regulation. Butyrate directly drives differentiation of colonic Foxp3⁺ regulatory T cells,^13,14 and a rationally selected Clostridia consortium has been shown to induce Tregs and attenuate colitis in vivo¹² — the template GR-201 is built on.

Candidate strains are mined from the GutRecover library by multi-omics-guided screening against validated colitis models, benchmarked to the IBD multi-omics reference.¹⁶ The goal is to deliver the remission signal seen with donor FMT in ulcerative colitis^9,10 in a defined, reproducible, manufacturable product.

Consortium composition

Representative functional classes of the GR-201 consortium, paired for butyrate output and Treg-inducing function. Exact isolates and ratios are proprietary.

Strain class	Functional role	Evidence
GRC-201·01	Faecalibacterium prausnitzii-class	Butyrate; anti-inflammatory (IL-10 / NF-κB) [15]
GRC-201·02	Roseburia intestinalis-class	Butyrate production [13]
GRC-201·03	Anaerostipes / Eubacterium rectale-class	Butyrogenic cross-feeding [13]
GRC-201·04	Clostridia clusters IV / XIVa	Foxp3⁺ Treg induction [12]
GRC-201·05	SCFA-responsive commensal	Peripheral Treg generation [23]

ModalityConsortium — discovery

Current stageDiscovery — target identification

Next milestoneDevelopment candidate nomination

Clinical trialIndication disclosed at IND

Mechanism

The gut microbiome programs systemic immune tone: defined commensal consortia can deterministically expand specific T-cell populations — an 11-strain consortium elicits IFN-γ⁺ CD8 T cells and anti-tumour immunity in vivo.¹⁸ GR-301 applies that principle to a chronic immune-mediated condition with a consistent, replicated microbiome signature.

Discovery is gated: GR-301 advances to development-candidate nomination only once gnotobiotic colonisation establishes a causal strain→immune-phenotype link meeting a pre-defined evidence threshold. The indication is disclosed at IND.

Consortium composition

GR-301 composition is undisclosed at the discovery stage. Design follows the published precedent that a defined multi-strain consortium can deterministically program systemic T-cell phenotypes; full composition is disclosed at development-candidate nomination / IND.

Strain class	Functional role	Evidence
Undisclosed	Defined consortium — CD8 / immune-tone programming	11-strain consortium elicits IFN-γ⁺ CD8 T cells [18]
—	Candidate set under gnotobiotic screening	Composition disclosed at IND [20]

// Programs shown at their honest development stage. Every scientific claim is sourced — see Publications.