Date published: 2025-9-28

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KLHL5 Inhibitors

KLHL5 inhibitors, as described above, primarily focus on the ubiquitin-proteasome system's modulation. KLHL5, a member of the Kelch-like protein family, has associations with ubiquitination and proteasomal degradation. By targeting this system, the indirect inhibitors can affect the function or stabilization of proteins KLHL5 might target. For instance, compounds like MG-132, Bortezomib, and Lactacystin hinder proteasomal activity, which prevents the degradation of ubiquitinated proteins. As KLHL5 is potentially involved in targeting proteins for degradation, these inhibitors can indirectly stabilize proteins that KLHL5 might ubiquitinate. Another dimension is added by inhibitors such as MLN4924, which disrupts the neddylation process essential for cullin-RING ligase function. Since Kelch-like proteins can be components of cullin-RING ligase complexes, this can modulate the ubiquitination activity of KLHL5. Furthermore, global disruptors of ubiquitination, like PYR-41 and TAK-243, can impact the overall ubiquitination landscape in cells, which includes processes that KLHL5 might oversee. Through these chemicals, one can navigate the complex ubiquitination machinery and potentially influence KLHL5's activity or its associated pathways.

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