Whole-Genome Profiles of Malay Colorectal Cancer Patients with Intact MMR Proteins

Author:

Juhari Wan Khairunnisa Wan,Ahmad Amin Noordin Khairul Bariah,Zakaria Andee DzulkarnaenORCID,Rahman Wan Faiziah Wan AbdulORCID,Mokhter Wan Muhamad Mokhzani Wan Muhamad,Hassan Muhammad Radzi Abu,Sidek Ahmad Shanwani Mohammed,Zilfalil Bin Alwi

Abstract

Background: This study aimed to identify new genes associated with CRC in patients with normal mismatch repair (MMR) protein expression. Method: Whole-genome sequencing (WGS) was performed in seven early-age-onset Malay CRC patients. Potential germline genetic variants, including single-nucleotide variations and insertions and deletions (indels), were prioritized using functional and predictive algorithms. Results: An average of 3.2 million single-nucleotide variations (SNVs) and over 800 indels were identified. Three potential candidate variants in three genes—IFNE, PTCH2 and SEMA3D—which were predicted to affect protein function, were identified in three Malay CRC patients. In addition, 19 candidate genes—ANKDD1B, CENPM, CLDN5, MAGEB16, MAP3K14, MOB3C, MS4A12, MUC19, OR2L8, OR51Q1, OR51AR1, PDE4DIP, PKD1L3, PRIM2, PRM3, SEC22B, TPTE, USP29 and ZNF117—harbouring nonsense variants were prioritised. These genes are suggested to play a role in cancer predisposition and to be associated with cancer risk. Pathway enrichment analysis indicated significant enrichment in the olfactory signalling pathway. Conclusion: This study provides a new spectrum of insights into the potential genes, variants and pathways associated with CRC in Malay patients.

Funder

Universiti Sains Malaysia

Publisher

MDPI AG

Subject

Genetics(clinical),Genetics

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