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Latent-TGF-β has a domain swapped architecture

Nature Communications. 2025-11; 
Mingliang Jin, Robert I Seed, Tiffany Shing, Li Wang, Junrui Li, Yifan Cheng, Stephen L Nishimura Department of Pathology, University of California San Francisco
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Catalog Antibodies Stable transfection of these lines with a HA-GARP construct (blastacidin resistance cassette) resulted in L-TGF-β surface expression, which was enhanced by selection and sorting to achieve high surface expression of TGF-β1/GARP or TGF-β1 (R249A)/GARP, as measured by anti-HA (clone 5E11D8, GenScript, Piscataway, NJ) or anti-LAP (R&D Systems, AF426). Get A Quote

摘要

The multifunctional cytokine TGF-β is a dimeric protein produced within a latent complex (L-TGF-β). Latency is maintained by disulfide linked homodimeric prodomains forming a ring encircling the non-covalently bound mature TGF-β homodimer. This configuration sterically inhibits mature TGF-β from binding to its receptors. For TGF-β to be activated and bind to its receptors it must either be released, or if not released, overcome steric hinderance within the latent complex. Integrin binding to L-TGF-β results in activation with or without release of TGF-β by deforming the ring through different yet incompletely understood mechanisms. The domain architecture of L-TGF-β, which is not clearly defined, is a g... More

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