AI Article Synopsis
- Researchers discovered a new glucocorticoid receptor modulator (GRM) that uses a thioester payload, designed to be quickly processed by the liver to reduce overall exposure in the body.
- This new payload clears from the system 10 times faster than earlier versions, leading to much lower drug levels and less risk of systemic effects.
- The antibody-drug conjugate demonstrated significant effectiveness in reducing inflammation in various mouse models, indicating potential for effective subcutaneous administration and applications in treating inflammatory diseases.
Article Abstract
We describe the discovery of a thioester-containing glucocorticoid receptor modulator (GRM) payload and the corresponding antibody-drug conjugate (ADC). Payload was designed for rapid hepatic inactivation to minimize systemic exposure of nonconjugated GRM. Mouse PK indicated that is cleared 10-fold more rapidly than a first-generation GRM payload, resulting in 10-fold lower exposure and 3-fold decrease in Cmax. The anti-mTNF conjugate fully inhibited inflammation in mouse contact hypersensitivity with minimal effects on corticosterone, a biomarker for systemic GRM effects, at doses up to and including 100 mg/kg. Concomitant inhibition of P1NP suggests potential delivery to cells involved in the remodeling of bone, which may be a consequence of TNF-targeting or bystander payload effects. Furthermore, fully suppressed inflammation in collagen-induced arthritis mouse model after one 10 mg/kg dose for 21 days. The properties of the anti-hTNF conjugate were suitable for liquid formulation and may enable subcutaneous dosing.
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| http://dx.doi.org/10.1021/acs.jmedchem.4c00598 | DOI Listing |
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