SALL4B, not targeted by IMiD, is important for SALL4-mediated tumorigenesis-Reference-Cited by-同舟云学术

SALL4B, not targeted by IMiD, is important for SALL4-mediated tumorigenesis

Published:2023-07-07 Issue: Volume: Page:
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Author:

L. Vu Kim Anh,Kumari Kalpana,Liu Bee Hui,Gao Chong,Li Feng,Tang Jing Ping,Maddalo Danilo,Auld Douglas S.,Casalena Dominick E.,Tian Xi,Liu Miao,Bassal Mahmoud A.^ORCID,Moein Shiva,Iakovleva Viktoriia,Tan Justin L.,Stein Alicia J.,Zhou Qiling,Fischer Patrick D.,Sigua Logan H.,Qi Jun,Arthanari Haribabu,Tenen Daniel G.^ORCID,Chai Li^ORCID

Abstract

AbstractOncofetal transcription factor SALL4 is essential for cancer cell survival.1-5Recently, several groups reported that immunomodulatory imide drugs (IMiDs) could degrade SALL4 in a proteasome-dependent manner.6,7Intriguingly, we observed that IMiDs had no effect on SALL4-positive cancer cells. Further studies demonstrated that IMiDs could only degrade SALL4A, one of the SALL4 isoforms. This finding raises the possibility that SALL4B, the isoform not affected by IMiDs, may be essential for SALL4-mediated cancer cell survival. SALL4B knockdown led to an increase in apoptosis and inhibition of cancer cell growth. SALL4B gain-of-function alone led to liver tumor formation in mice. Our observation that protein degraders can possess isoform-specific effects exemplifies the importance of delineating drug action and oncogenesis at the isoform level to develop more effective cancer therapeutics.

Publisher

Cold Spring Harbor Laboratory

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5. SALL4 promotes gastric cancer progression through activating CD44 expression