A Novel Inhibitor for Krasg12c Mutant Lung Carcinoma
No Thumbnail Available
Date
2020
Authors
Kanbur, Tuğçe
Çağır, Ali
Journal Title
Journal ISSN
Volume Title
Publisher
International Association for the Study of Lung Cancer
Open Access Color
OpenAIRE Downloads
OpenAIRE Views
Abstract
Mutations in KRAS are among the most common aberrations
in cancer. However, despite considerable research efforts, KRAS
remains a challenging therapeutic target. In recent years, there has
been a drive to develop KRAS mutant specific drugs. Among the
different known mutations, the KRASG12C (glycine 12 to cysteine) has
been considered druggable. Studies have shown that due in part to the
close proximity of Cysteine 12 to both the nucleotide pocket and the
switch regions, thiol-reactive compounds can bind to the active site
covalently and inhibit KRASG12C mutation-driven signaling. The
absence of this particular cysteine residue in wild-type KRAS makes
such an approach very selective towards cancer cells.
Description
Keywords
KRAS, Lung cancer
Turkish CoHE Thesis Center URL
Fields of Science
Citation
WoS Q
Q1
Scopus Q
Q1
Source
Journal of Thoracic Oncology
Volume
15
Issue
2
Start Page
S15
End Page
S15
Sustainable Development Goals
3
GOOD HEALTH AND WELL-BEING
9
INDUSTRY, INNOVATION AND INFRASTRUCTURE
