Skip NavigationSkip to Content
Return Return to Search Results

Abrogation of the G2/M checkpoint as a chemo sensitization approach for alkylating agents

  1. Author:
    Lang, Fengchao
    Cornwell, James A
    Kaur, Karambir
    Elmogazy, Omar
    Zhang, Wei
    Zhang, Meili
    Song, Hua
    Sun,David
    Wu,Xiaolin [ORCID]
    Aladjem, Mirit I
    Aregger,Michael
    Cappell, Steven D
    Yang, Chunzhang [ORCID]

  2. Author Address

    Neuro-Oncology Branch, Center for Cancer Research, National Cancer Institute, MD., Laboratory of Cancer Biology and Genetics, Center for Cancer Research, National Cancer Institute, MD., Cancer Research Technology Program, Frederick National Laboratory for Cancer Research, MD., Developmental Therapeutics Branch, Center for Cancer Research, National Cancer Institute, MD., Molecular Targets Program, Center for Cancer Research, National Cancer Institute, MD.,
    1. Year: 2023
    2. Date: Dec 22
    3. Epub Date: 2023 12 22
  2. Journal: Neuro-Oncology
  4. Type of Article: Article
  1. Abstract:

    The cell cycle is tightly regulated by checkpoints, playing a vital role in controlling its progression and timing. Cancer cells exploit the G2/M checkpoint, which serves as a resistance mechanism against genotoxic anti-cancer treatments, allowing for DNA repair prior to cell division. Manipulating cell cycle timing has emerged as a potential strategy to augment the effectiveness of DNA damage-based therapies. In this study, we conducted a forward genome wide CRISPR/Cas9 screening with repeated exposure to the alkylating agent temozolomide (TMZ) to investigate the mechanisms underlying tumor cell survival under genotoxic stress. Our findings revealed that canonical DNA repair pathways, including ATM/Fanconi and mismatch repair, determine cell fate under genotoxic stress. Notably, we identified the critical role of PKMYT1, in ensuring cell survival. Depletion of PKMYT1 led to overwhelming TMZ-induced cytotoxicity in cancer cells. Isobologram analysis demonstrated potent drug synergy between alkylating agents and a Myt1 kinase inhibitor, RP-6306. Mechanistically, inhibiting Myt1 forced G2/M-arrested cells into an unscheduled transition to the mitotic phase without complete resolution of DNA damage. This forced entry into mitosis, along with persistent DNA damage, resulted in severe mitotic abnormalities. Ultimately, these aberrations led to mitotic exit with substantial apoptosis. Preclinical animal studies demonstrated that the combination regimen involving TMZ and RP-6306 prolonged the overall survival of glioma-bearing mice. Collectively, our findings highlight the potential of targeting cell cycle timing through Myt1 inhibition as an effective strategy to enhance the efficacy of current standard cancer therapies, potentially leading to improved disease outcomes. Published by Oxford University Press on behalf of the Society for Neuro-Oncology 2023. This work is written by (a) US Government employee(s) and is in the public domain in the US.

    See More

  1. Keywords:

External Sources

  1. View Full Text
  2. DOI: 10.1093/neuonc/noad252
  3. PMID: 38134889
  4. PII : 7491950

Library Notes

  1. Fiscal Year: FY2023-2024
NCI at Frederick

You are leaving a government website.

This external link provides additional information that is consistent with the intended purpose of this site. The government cannot attest to the accuracy of a non-federal site.

Linking to a non-federal site does not constitute an endorsement by this institution or any of its employees of the sponsors or the information and products presented on the site. You will be subject to the destination site's privacy policy when you follow the link.

ContinueCancel