Targeting Werner Syndrome Helicase with Small Molecules in Mismatch Repair-Deficient Cancers.

Journal: ACS Medicinal Chemistry Letters
Published:
Abstract

Recent efforts have identified WRN helicase as a critical dependency in mismatch repair-deficient (dMMR) cancers. Small molecules targeting WRN demonstrate selective activity in microsatellite instability-high (MSI-H) models. These compounds impair tumor growth and promote cancer cell death by disrupting genome maintenance pathways, highlighting a promising therapeutic strategy for genetically defined, treatment-resistant tumors.

Authors
Robert Kargbo
Relevant Conditions

Werner Syndrome

Similar Publications

The Werner syndrome helicase is a cofactor for HIV-1 long terminal repeat transactivation and retroviral replication.
The Werner syndrome helicase is a cofactor for HIV-1 long terminal repeat transactivation and retroviral replication.
Journal: The Journal of biological chemistry
Published: February 24, 2007
WRN helicase expression in Werner syndrome cell lines.
WRN helicase expression in Werner syndrome cell lines.
Journal: Nucleic acids research
Published: December 22, 1999
DNA damage-induced translocation of the Werner helicase is regulated by acetylation.
DNA damage-induced translocation of the Werner helicase is regulated by acetylation.
Journal: The Journal of biological chemistry
Published: October 18, 2002
View All