POLD1 DEDD Motif Mutation Confers Hypermutation in Endometrial Cancer and Durable Response to Pembrolizumab

Christina Hsiao Wei; Edward Wenge Wang; Lingzi Ma; Yajing Zhou; Li Zheng; Heather Hampel; Susan Shehayeb; Stephen Lee; Joshua Cohen; Adrian Kohut; Fang Fan; Steven Rosen; Xiwei Wu; Binghui Shen; Yuqi Zhao

doi:10.3390/cancers15235674

POLD1 DEDD Motif Mutation Confers Hypermutation in Endometrial Cancer and Durable Response to Pembrolizumab

Cancers (Basel). 2023 Nov 30;15(23):5674. doi: 10.3390/cancers15235674.

Authors

Christina Hsiao Wei¹, Edward Wenge Wang², Lingzi Ma³, Yajing Zhou³, Li Zheng³, Heather Hampel⁴, Susan Shehayeb⁴, Stephen Lee⁵, Joshua Cohen⁵, Adrian Kohut⁵, Fang Fan¹, Steven Rosen^{6

7}, Xiwei Wu⁷, Binghui Shen³, Yuqi Zhao⁷

Affiliations

¹ Department of Pathology, City of Hope Medical Center (COHNMC), Duarte, CA 91010, USA.
² Department of Oncology & Therapeutics Research, City of Hope Medical Center (COHNMC), Duarte, CA 91010, USA.
³ Department of Cancer Genetics and Epigenetics, Beckman Research Institute at City of Hope Medical Center (COHNMC), Duarte, CA 91010, USA.
⁴ Clinical Cancer Genetics, City of Hope Medical Center (COHMC), Duarte, CA 91010, USA.
⁵ Division of Gynecologic Oncology and Surgery, City of Hope Medical Center (COHNMC), Duarte, CA 91010, USA.
⁶ Department of Hematology & Hematopoietic Cell Transplantation, City of Hope Medical Center (COHNMC), Duarte, CA 91010, USA.
⁷ Beckman Research Institute of City of Hope, Duarte, CA 91010, USA.

Abstract

Background: Mutations in the DNA polymerase delta 1 (POLD1) exonuclease domain cause DNA proofreading defects, hypermutation, hereditary colorectal and endometrial cancer, and are predictive of immunotherapy response. Exonuclease activity is carried out by two magnesium cations, bound to four highly conserved, negatively charged amino acids (AA) consisting of aspartic acid at amino acid position 316 (p.D316), glutamic acid at position 318 (p.E318), p.D402, and p.D515 (termed DEDD motif). Germline polymorphisms resulting in charge-discordant AA substitutions in the DEDD motif are classified as variants of uncertain significance (VUSs) by laboratories and thus would be considered clinically inactionable. We hypothesize this mutation class is clinically pathogenic.

Methods: A review of clinical presentation was performed in our index patient with a POLD1(p.D402N) heterozygous proband with endometrial cancer. Implications of this mutation class were evaluated by a Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA)-guided systematic review, in silico analysis with orthogonal biochemical confirmation, and whole-exome and RNA sequencing analysis of the patient's tumor and engineered cell lines.

Results: Our systematic review favored a Mendelian disease mutation class associated with endometrial and colorectal cancers. In silico analysis predicted defective protein function, confirmed by biochemical assay demonstrating loss of nuclease activity. A POLD1-specific mutational signature was found in both the patient's tumor and POLD1(p.D402N) overexpressing cell. Furthermore, paired whole-exome/transcriptome analysis of endometrial tumor demonstrated hypermutation and T cell-inflamed gene expression profile (GEP), which are joint predictive biomarkers for pembrolizumab. Our patient showed a deep, durable response to immune checkpoint inhibitor (ICI).

Conclusion: Charge-discordant AA substitution in the DEDD motif of POLD1 is detrimental to DNA proofreading and should be reclassified as likely pathogenic and possibly predictive of ICI sensitivity.

Keywords: DNA polymerase delta; POLD1; endometrial cancer; germline; hypermutation; immunotherapy; variant of uncertain significance.

Abstract

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