Catalase C262T genetic variation and cancer susceptibility: A comprehensive meta-analysis with meta-regression and trial sequential analysis

Md Abdul Barek; Sarah Jafrin; Md Abdul Aziz; Mohammad Safiqul Islam

doi:10.1177/03936155221104128

Catalase C262T genetic variation and cancer susceptibility: A comprehensive meta-analysis with meta-regression and trial sequential analysis

Int J Biol Markers. 2022 Sep;37(3):227-240. doi: 10.1177/03936155221104128. Epub 2022 May 30.

Authors

Md Abdul Barek^{1

2}, Sarah Jafrin^{1

2}, Md Abdul Aziz³, Mohammad Safiqul Islam^{1

2}

Affiliations

¹ Department of Pharmacy, Faculty of Science, 378872Noakhali Science and Technology University, Noakhali, Bangladesh.
² Laboratory of Pharmacogenomics and Molecular Biology, Department of Pharmacy, 378872Noakhali Science and Technology University, Noakhali, Bangladesh.
³ Department of Pharmacy, Faculty of Pharmacy and Health Sciences, 185960State University of Bangladesh, Dhaka, Bangladesh.

PMID: 35645161
DOI: 10.1177/03936155221104128

Abstract

Several genetic association studies have analyzed the link between the catalase (CAT) C262T variant and different cancers, but the findings remain controversial. Our research centered on establishing a comprehensive correlation between the C262T variant and different cancers. This study was conducted using RevMan 5.4 software following the PRISMA 2020 guidelines. For this meta-analysis, 53 case-control studies (18,258 cases and 47,476 controls) were chosen. The analysis revealed that three genetic models were statistically linked (P < 0.05) to overall cancer susceptibility in codominant model 2 (COD2): odds ratio (OR) = 1.16, COD3: OR = 1.21, recessive model (RM): OR = 1.20). After stratification by ethnicity, a significant link (P < 0.05) was found in Caucasians (COD2: OR = 1.18, COD3: OR = 1.17, over-dominant model (ODM): OR = 1.19) and Asians (COD3: OR = 1.49). Subgroup analyses revealed a significant correlation (P < 0.05) with blood-and-bone-marrow-related cancer, skin cancer, gastrointestinal-tract-related cancer, prostate cancer, and gynecologic cancer. Three genetic models in population-based controls (COD2: OR = 1.19, COD3: OR = 1.17, RM: OR = 1.19) and two genetic models in hospital-based controls (COD3: OR = 1.40, RM: OR = 1.24) were found to be significantly correlated (P < 0.05) with cancer. Also, three genetic models for polymerase chain reaction-restriction fragment length polymorphism (COD3: OR = 1.46; RM: OR = 1.34, ODM: OR = 0.80) and three models for MALDI-TOF + MassARRAY (COD2: OR = 1.32, RM: OR = 1.26, allele model: OR = 1.14) genotyping methods showed significant association (P < 0.05) with cancer. The meta-regression showed that the quality scores might be a source of significant heterogeneity under the COD2 model (coefficient = 0.176, P = 0.029). Trial sequential analysis also validated the adequacy of the sample size on overall findings. Our results indicate that CAT C262T variant is associated with overall cancer susceptibility, especially in Caucasians and Asians. This variant may also be associated with blood-and-bone-marrow-related, GIT-related, prostate, skin, and gynecological cancers.

Keywords: CAT C262T; Cancer; Catalase; Meta-analysis; Polymorphism.

Publication types

Meta-Analysis

MeSH terms

Case-Control Studies
Catalase / genetics
Female
Gastrointestinal Neoplasms*
Genetic Predisposition to Disease*
Humans
Polymorphism, Single Nucleotide
Retinitis Pigmentosa
Risk Factors

Substances

Catalase

Supplementary concepts

Cone Dystrophy 3