Slow<i>N</i>‐acetylation as a possible contributor to bladder carcinogenesis

Kawak, Michelle El; Dhaini, Hassan R.; Jabbour, Michel E.; Moussa, Mohamad; Asmar, Khalil El; Aoun, Mona

doi:10.1002/mc.23232

Cited by 15 publications

(8 citation statements)

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“…In this analysis, we report on potential risk modification of the relation between THM exposure and 16 loci associated with bladder cancer. Although there is evidence that

-acetyltransferase 1 (NAT1) also plays a role in bladder carcinogenesis, 26 SNPs in NAT1 genotyped as part of our GWAS did not show strong evidence of association with bladder cancer risk and therefore is not presented in these results. We found the strongest evidence of such an association for rs907611 ( LSP1 region), with a suggestion of interaction in both New England and Spain.…”

Section: Discussionmentioning

confidence: 81%

Disinfection By-Products in Drinking Water and Bladder Cancer: Evaluation of Risk Modification by Common Genetic Polymorphisms in Two Case–Control Studies

Freeman

Kogevinas

Cantor

et al. 2022

Environ Health Perspect

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Background: By-products are formed when disinfectants react with organic matter in source water. The most common class of disinfection by-products, trihalomethanes (THMs), have been linked to bladder cancer. Several studies have shown exposure–response associations with THMs in drinking water and bladder cancer risk. Few epidemiologic studies have evaluated gene–environment interactions for total THMs (TTHMs) with known bladder cancer susceptibility variants. Objectives: In this study, we investigated the combined effect on bladder cancer risk contributed by TTHMs, bladder cancer susceptibility variants identified through genome-wide association studies, and variants in several candidate genes. Methods: We analyzed data from two large case–control studies—the New England Bladder Cancer Study ( cases/1,162 controls), a population-based study, and the Spanish Bladder Cancer Study ( cases/772 controls), a hospital-based study. Because of differences in exposure distributions and metrics, we estimated effects of THMs and genetic variants within each study separately using adjusted logistic regression models to calculate odds ratios (ORs) and 95% confidence intervals (CI) with and without interaction terms, and then combined the results using meta-analysis. Results: Of the 16 loci showing strong evidence of association with bladder cancer, rs907611 at 11p15.5 [leukocyte-specific protein 1 ( LSP1 region)] showed the strongest associations in the highest exposure category in each study, with evidence of interaction in both studies and in meta-analysis. In the highest exposure category, we observed (95% CI: 1.17, 2.34, ) for those with the rs907611-GG genotype and . No other genetic variants tested showed consistent evidence of interaction. Discussion: We found novel suggestive evidence for a multiplicative interaction between a putative bladder carcinogen, TTHMs, and genotypes of rs907611. Given the ubiquitous exposure to THMs, further work is needed to replicate and extend this finding and to understand potential molecular mechanisms. https://doi.org/10.1289/EHP9895

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“…In this analysis, we report on potential risk modification of the relation between THM exposure and 16 loci associated with bladder cancer. Although there is evidence that

Section: Discussionmentioning

confidence: 81%

Disinfection By-Products in Drinking Water and Bladder Cancer: Evaluation of Risk Modification by Common Genetic Polymorphisms in Two Case–Control Studies

Freeman

Kogevinas

Cantor

et al. 2022

Environ Health Perspect

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“…Notably, the incidence of urinary bladder cancer has increased markedly in Lebanon and is currently the second most incident cancer among males ( Shamseddine et al, 2004 ). The frequency of 560G > A (rs4986782) (R187Q) is 7-fold higher among urinary bladder cases than controls in Lebanon ( Yassine et al, 2012 ) and is significantly associated with higher muscle-invasiveness and higher tumor grade of urinary bladder tumors ( El Kawak et al, 2020 ). In the current study 560G > A (rs4986782) (R187Q) caused a 4 to 5-fold increase ( p < 0.05) in affinity for both ABP and N-OH-ABP.…”

Section: Discussionmentioning

confidence: 99%

“…Most of these focus on associations between NAT1*10 and/or NAT1*11 and cancer risk, two variant alleles that possess SNPs in the 3′-UTR region outside of the coding exon. Urinary bladder cancer is most frequently associated with NAT1 genetic polymorphism ( Cascorbi et al, 2001 ; Yassine et al, 2012 ; Dhaini et al, 2018 ; El-Kawak et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

560G>A (rs4986782) (R187Q) Single Nucleotide Polymorphism in Arylamine N-Acetyltransferase 1 Increases Affinity for the Aromatic Amine Carcinogens 4-Aminobiphenyl and N-Hydroxy-4-Aminobiphenyl: Implications for Cancer Risk Assessment

Doll

Hein

2022

Front. Pharmacol.

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Human arylamine N-acetyltransferase 1 (NAT1) catalyzes the N-acetylation of arylamine carcinogens such as 4-aminobiphenyl (ABP), and following N-hydroxylation, the O-acetylation of N-hydroxy-arylamine carcinogens such as N-hydroxy-ABP (N-OH-ABP). Genetic polymorphisms in NAT1 are linked to cancer susceptibility following exposures. The effects of individual single nucleotide polymorphisms (SNPs) in the NAT1 coding exon on Michaelis-Menten kinetic constants was assessed for ABP N-acetyltransferase and N-OH-ABP O-acetyltransferase activity following transfection of human NAT1 into COS-1 cells (SV40-transformed African green monkey kidney cells). NAT1 coding region SNPs 97C > T (rs56318881) (R33stop), 190C > T (rs56379106) (R64W), 559C > T (rs5030839) (R187stop) and 752A > T (rs56172717) (D251V) reduced ABP N- acetyltransferase and N-OH-ABP O-acetyltransferase activity below detection. 21T > G (rs4986992) (synonymous), 402T > C (rs146727732) (synonymous), 445G > A (rs4987076) (V149I), 613A > G (rs72554609) (M205V) and 640T > G (rs4986783) (S241A) did not significantly affect Vmax for ABP N-acetyltransferase or N-OH-ABP O-acetyltransferase. 781G > A (rs72554610) (E261K), and 787A > G (rs72554611) (I263V) slightly reduced ABP N-acetyltransferase and N-OH-ABP O-acetyltransferase activities whereas 560G > A (rs4986782) (R187Q) substantially and significantly reduced them. 560G > A (rs4986782) (R187Q) significantly reduced the apparent Km for ABP and N-OH-ABP a finding that was not observed with any of the other NAT1 SNPs tested. These findings suggest that the role of the 560G > A (rs4986782) (R187Q) SNP cancer risk assessment may be modified by exposure level to aromatic amine carcinogens such as ABP.

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“…Studies have shown that N-acetylation mainly affects protein-membrane binding and protein stability ( 16 ). N-acetylation is also one of many factors contributing to tumor progression; for example, slow N-acetylation is a factor in bladder carcinogenesis and muscle invasiveness, and NAT1 is recognized as a biomarker candidate in bladder cancer and a potential target for drug development point ( 17 ).…”

Section: The Components and Process Of Acetylation System In Cancersmentioning

confidence: 99%

The role of protein acetylation in carcinogenesis and targeted drug discovery

2022

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Protein acetylation is a reversible post-translational modification, and is involved in many biological processes in cells, such as transcriptional regulation, DNA damage repair, and energy metabolism, which is an important molecular event and is associated with a wide range of diseases such as cancers. Protein acetylation is dynamically regulated by histone acetyltransferases (HATs) and histone deacetylases (HDACs) in homeostasis. The abnormal acetylation level might lead to the occurrence and deterioration of a cancer, and is closely related to various pathophysiological characteristics of a cancer, such as malignant phenotypes, and promotes cancer cells to adapt to tumor microenvironment. Therapeutic modalities targeting protein acetylation are a potential therapeutic strategy. This article discussed the roles of protein acetylation in tumor pathology and therapeutic drugs targeting protein acetylation, which offers the contributions of protein acetylation in clarification of carcinogenesis, and discovery of therapeutic drugs for cancers, and lays the foundation for precision medicine in oncology.

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SlowN‐acetylation as a possible contributor to bladder carcinogenesis

Cited by 15 publications

References 50 publications

Disinfection By-Products in Drinking Water and Bladder Cancer: Evaluation of Risk Modification by Common Genetic Polymorphisms in Two Case–Control Studies

Disinfection By-Products in Drinking Water and Bladder Cancer: Evaluation of Risk Modification by Common Genetic Polymorphisms in Two Case–Control Studies

560G>A (rs4986782) (R187Q) Single Nucleotide Polymorphism in Arylamine N-Acetyltransferase 1 Increases Affinity for the Aromatic Amine Carcinogens 4-Aminobiphenyl and N-Hydroxy-4-Aminobiphenyl: Implications for Cancer Risk Assessment

The role of protein acetylation in carcinogenesis and targeted drug discovery

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