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DGAT2 Target Evaluation Report: Biology, Validation, Competition, IP, and R&D Strategy

13 July 2026
8 min read

PatSnap Open Platform

This Target Evaluation Report for DGAT2 is generated from PatSnap Life Sciences MCP data workflows, combining Target & Disease MCP biology context with Clinical Trials MCP validation and competitive signals.

For AI teams building biomedical agents, PatSnap Life Sciences MCP Servers provide structured retrieval across target biology, disease context, clinical trials, drug evidence, IP intelligence, and other R&D intelligence sources.

20

Direct drug records from Target & Disease MCP

12

Development records in target context

21

Disease associations captured

26

Clinical trial records from Clinical Trials MCP

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Executive View

Biology signal

DGAT2 is evaluated using the DGAT2 family evidence returned by Target & Disease MCP. The family sits in the final triglyceride synthesis pathway, complementary to DGAT1, and is relevant where hepatic lipid storage, obesity, and metabolic-disease biology intersect.

Validation evidence

MCP retrieval returned 20 drug records, 12 development records, and 21 disease associations on a roll-up basis. Clinical Trials MCP returned 26 trial records, including S-309309 Phase 1 pharmacokinetic and mass-balance studies plus a Phase 2 obesity study.

Competition and differentiation

DGAT2 is less clinically crowded than broad lipid targets, but translation requires solving tissue exposure and metabolic tolerability. Programs should be compared on liver selectivity, triglyceride effects, weight/metabolic endpoints, and safety monitoring.

IP and partnering view

IP diligence should focus on chemistry, hepatic targeting, obesity or MASH-related use claims, and whether the candidate can be separated from earlier DGAT liabilities. Platform partnerships may matter if delivery or tissue exposure is the differentiator.

Clinical Validation and Competitive Landscape

Clinical Trials MCP returned 26 registered trial records connected to DGAT2. The sample below is used as a directional competitive readout rather than a full regulatory review.

TrialPhaseStatus
Effect of itraconazole on the pharmacokinetics of S-309309 in healthy participantsPhase 1Completed
Safety and efficacy study of S-309309 in obese adultsPhase 2Completed
Mass balance study of [14C]S-309309 oral capsule in healthy adult male participantsPhase 1No longer recruiting

R&D Strategy Recommendation

DGAT2 is a focused metabolic target with a moderate evidence base. Advance only where a program has a clear liver/metabolic rationale and a safety thesis that can withstand comparison with DGAT1 and broader lipid-modulating strategies.

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