Rad5 and Its Human Homologs, HLTF and SHPRH, Are Novel Interactors of Mismatch Repair

Miller, Anna Kristin; Mao, Guogen; Knicely, Breanna G.; Daniels, Hannah G.; Rahal, Christine M.; Putnam, Christopher D.; Kolodner, Richard D.; Goellner, Eva M.

doi:10.3389/fcell.2022.843121

Cited by 4 publications

(1 citation statement)

References 64 publications

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“…6e). Interestingly, SHPRH is known to interact with DNA replication components, transcription factors and RNA polymerase, and along with its paralog HLTF, has recently been demonstrated to have roles in various DNA repair pathways in addition to template switching including MMR and NER, further supporting these findings [74][75][76][77][78].…”

Section: Re-expression Of Shprh In Lung Adenocarcinoma Cells With Ina...mentioning

confidence: 75%

Integrative genomics identifies SHPRH as a tumor suppressor gene in lung adenocarcinoma that regulates DNA damage response

Nagelberg,

Sihota,

Chuang

et al. 2024

Br J Cancer

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Background Identification of driver mutations and development of targeted therapies has considerably improved outcomes for lung cancer patients. However, significant limitations remain with the lack of identified drivers in a large subset of patients. Here, we aimed to assess the genomic landscape of lung adenocarcinomas (LUADs) from individuals without a history of tobacco use to reveal new genetic drivers of lung cancer. Methods Integrative genomic analyses combining whole-exome sequencing, copy number, and mutational information for 83 LUAD tumors was performed and validated using external datasets to identify genetic variants with a predicted functional consequence and assess association with clinical outcomes. LUAD cell lines with alteration of identified candidates were used to functionally characterize tumor suppressive potential using a conditional expression system both in vitro and in vivo. Results We identified 21 genes with evidence of positive selection, including 12 novel candidates that have yet to be characterized in LUAD. In particular, SNF2 Histone Linker PHD RING Helicase (SHPRH) was identified due to its frequency of biallelic disruption and location within the familial susceptibility locus on chromosome arm 6q. We found that low SHPRH mRNA expression is associated with poor survival outcomes in LUAD patients. Furthermore, we showed that re-expression of SHPRH in LUAD cell lines with inactivating alterations for SHPRH reduces their in vitro colony formation and tumor burden in vivo. Finally, we explored the biological pathways associated SHPRH inactivation and found an association with the tolerance of LUAD cells to DNA damage. Conclusions These data suggest that SHPRH is a tumor suppressor gene in LUAD, whereby its expression is associated with more favorable patient outcomes, reduced tumor and mutational burden, and may serve as a predictor of response to DNA damage. Thus, further exploration into the role of SHPRH in LUAD development may make it a valuable biomarker for predicting LUAD risk and prognosis.

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Section: Re-expression Of Shprh In Lung Adenocarcinoma Cells With Ina...mentioning

confidence: 75%

Integrative genomics identifies SHPRH as a tumor suppressor gene in lung adenocarcinoma that regulates DNA damage response

Nagelberg,

Sihota,

Chuang

et al. 2024

Br J Cancer

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The fork remodeler helicase-like transcription factor in cancer development: all at once

Waheed,

Mojumdar,

Shafiq

et al. 2024

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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HLTF resolves G4s and promotes G4-induced replication fork slowing to maintain genome stability

Bai,

Endres,

Kühbacher

et al. 2024

Molecular Cell

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Rad5 and Its Human Homologs, HLTF and SHPRH, Are Novel Interactors of Mismatch Repair

Cited by 4 publications

References 64 publications

Integrative genomics identifies SHPRH as a tumor suppressor gene in lung adenocarcinoma that regulates DNA damage response

Integrative genomics identifies SHPRH as a tumor suppressor gene in lung adenocarcinoma that regulates DNA damage response

The fork remodeler helicase-like transcription factor in cancer development: all at once

HLTF resolves G4s and promotes G4-induced replication fork slowing to maintain genome stability

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