Chemical inhibitors of Vrho operate through various mechanisms to halt its protease activity. E-64, due to its capacity to covalently bind with cysteine residues within protease active sites, effectively hampers the proteolytic function of Vrho. Similarly, Leupeptin targets serine and cysteine proteases, forming a stable complex that hinders the enzyme's activity, thereby restricting Vrho's proteolytic actions. Pepstatin A is known for its inhibition of aspartyl proteases by docking into their active sites, a mechanism that can extend to the protease domain of Vrho, assuming it shares structural similarity. Chymostatin's specificity towards chymotrypsin-like serine proteases enables it to suppress similar activities within Vrho, provided that Vrho exhibits comparable serine protease behavior.
Phosphoramidon, by latching onto the zinc-binding motifs of metalloproteases, can suppress metalloprotease-like activity, which may include the functions of Vrho. MG-132 interrupts proteasome and protease activities by modifying active site threonine residues, a process that can inhibit Vrho's protease function. Lactacystin's irreversible inhibition of proteasomal proteolytic function would similarly affect Vrho if its proteolytic mechanism is akin to that of the proteasome. Aprotinin's inhibition spectrum, while focused primarily on trypsin-like enzymes, would extend to Vrho. Marimastat, as a broad-spectrum metalloprotease inhibitor, can impede Vrho by binding to any potential metalloprotease domain within the protein. Ilomastat, another metalloprotease inhibitor, would inhibit Vrho by sequestering the zinc ion at the metalloprotease active site, assuming Vrho's activity depends on such a metal ion. Calpeptin, targeting calpain or similar calcium-dependent proteases, would inhibit Vrho. Lastly, CA-074 selectively inhibits cathepsin B-like cysteine proteases, which would extend to Vrho, restraining its proteolytic capability.
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