Relationship between XPD, RAD51, and APEX1 DNA repair genotypes and prostate cancer risk in the male population of Rio de Janeiro, Brazil

Cypriano, Ana Sheila; Alves, Gilda; Ornellas, Antonio Augusto; Scheinkman, José; Almeida, Renata; Scherrer, Luciano; Lage, Claudia

doi:10.1590/1678-4685-GMB-2017-0039

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Genetics and Molecular Biology

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Human and Medical Genetics • Genet. Mol. Biol. 40 (4) • Oct-Dec 2017 • https://doi.org/10.1590/1678-4685-GMB-2017-0039 copy

Relationship between XPD, RAD51, and APEX1 DNA repair genotypes and prostate cancer risk in the male population of Rio de Janeiro, Brazil

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Susceptibility to cancer ensues in individuals carrying malfunctioning DNA repair mechanisms. The impact of Single Nucleotide Polymorphisms (SNPs) in key DNA repair mechanisms on risk for prostate cancer was investigated in this case-control study. Samples consisted of 110 patients with confirmed prostate cancer and 200 unaffected men, from Rio de Janeiro, Brazil. XPD/Lys751Gln (rs13181), APEX1/Asp148Glu (rs1130409), and RAD51/G135C (rs1801320) SNPs were analyzed by PCR-RFLP. Allelic and genotypic frequencies were calculated and compared by Chi-Square test. The association between SNPs and clinical/epidemiological data was considered significant by Odds Ratio analysis, with IC95% and a p-value≤0.05. Only the XPD/Lys751Gln SNP significantly increased susceptibility to disease in southeastern Brazilian men, with p≤0.001 [OR=2.36 (1.46-3.84)], with no association with APEX1 or RAD51 SNPs. Combined XPD+RAD51 SNPs were highly associated with the disease, p≤0.005 [OR=3.40 (1.32-9.20)]. A Chi-Square significant association between XPD/Lys751Gln and Gleason score was also observed (OR=9.31; IC95%=1.19–428.0; p=0.022). Epidemiological inquiries revealed that exposure to pesticides significantly impacted the risk for prostate cancer in this population. DNA repair dysfunctions seem to prevail among workers exposed to chemical byproducts to cancer in this specific tissue. Non-invasive genotyping SNPs may help assessment of prostate cancer risk in environmentally exposed populations.

Keywords:
Prostate cancer; single nucleotide polymorphism; XPD; DNA repair; gene-environment interaction

Risk Factors	Groups		p value
	Controls, n (%)	Cases, n (%)
Organic solvents	43 (21.3)	9 (8.3)
Chronic diseases	91 (45.7)	45 (41.3)
Pesticides	7 (3.5)	23 (21.1) ^a a this particular environmental agent was highly significant (p < 0.05) in terms of risk for prostate cancer in exposed men.
Combustion products	5 (2.5)	10 (9.2)	p < 0.0001
Combustion + solvent	3 (1.5)	1 (0.9)
None	50 (25.2)	21 (19.2)
Totals	199^* * each patient was allocated in just one category, the one to which he declared to have been exposed to for longer periods. (100)	109^* * each patient was allocated in just one category, the one to which he declared to have been exposed to for longer periods. (100)

	XPD			RAD51			APEX1
Clinical record	wild-type	polymorphic	OR	wild-type	polymorphic	OR	wild-type	polymorphic	OR
			(95% CI)			(95% CI)			(95% CI)
Age (n=110)
			0.82			0.47			0.90
			(0.32 - 2.04)			(0.17 - 1.28)			(0.37 - 2.21)
< 60	12(30%)	24(34.3%)	X²=0.212	24(28.6%)	12(46.2%)	X²=2.788	21(31.8%)	15(34.1%)	X²=0.062
			p=0.645			p=0.095			p=0.804
> 60	28(70%)	46(65.7%)		60(71.4%)	14(53.8%)		45(68.2%)	29(65.9%)
Prognosis (n=43)			X²=3.055 p=0.217
Good	1(11.2%)	5(14.3%)		5(13.9%)	1(14.3%)	X²=6.954	2(9.5%)	4(18.2%)	X²=0.897
Bad	4(44.4%)	24(68.6%)		26(72.2%)	2(28.6%)	p=0.031	15(71.4%)	13(59.1%)	p=0.638
Uncertain	4(44.4%)	6(17.1%)		5(13.9%)	4(57.1%)		4(19.1%)	5(22.7%)
Gleason Score (n=57)
			9.31			0.40			1.13
			(1.19 – 428.0)			(0.06 - 1.85)			(0.33 - 3.82)
			X²=5.907			X²=1.711			X²=0.053
< 7	15(93.8%)	25(61%)	p=0.015	25(56.8%)	10(76.9%)	p=0.191	20(64.5%)	16(61.5%)	p=0.816
≥ 7	1(6.2%)	16(39%)		19(43.2%)	3(23.1%)		11(35.5%)	10(38.5%)
PSA (n=79)
			1.74			0.53			0.57
			(0.54 - 5.46)			(0.17 - 1.64)			(0.19 - 1.69)
			X²=1.174			X²=1.600			X²=1.289
< 5ng/mL	9(39.1%)	15(26.8%)	p=0.278	14(25.9%)	10(40%)	p=0.206	12(25.5%)	12(37.5%)	p=0.256
≥ 5ng/mL	14(60.9%)	41(73.2%)		40(74.1%)	15(60%)		35(74.5%)	20(62.5%)

	XPD			RAD51			APEX1			Totals
	A\|A	A\|C	C\|C	G\|G	G\|C	C\|C	T\|T	T\|G	G\|G
Patients n (%)	40 (36.4)	55 (50.0)	15 (13.6)	84 (76.4)	24 (21.8)	2 (1.8)	66 (60.0)	33 (30.0)	11 (10.0)	110
										(100)
Control group n (%)	115 (57.5)	68 (34.0)	17 (8.5)	157 (78.5)	40 (20.0)	3 (1.5)	114 (57.0)	84 (42.0)	2 (1.0)	200 (100)
Totals	155 (50.0)	123 (39.7)	32 (10.3)	241 (77.7)	64 (20.6)	5 (1.6)	180 (58.1)	117 (37.7)	13 (4.2)	310 (100)
OR		2.36			1.13			0.88
		(1.46 – 3.84)			(0.64 – 1.96)			(0.55 – 1.42)
(95% CI)		p <0.001			p=0.766			p=0.696
Hardy-Weinberg Equilibrium		p=0.345			p=0.788			p=0.337

Parameters	Probabilities
	XPD	RAD51	APEX1	XPD + RAD51
Sensitivity (%)	63.6 (54.3-72.0)	23.6 (16.7-32.4)	40.0 (31.3-49.3)	62.1 (44.0-77.3)
Specificity (%)	57.5 (50.5-64.1)	78.5 (72.3-83.6)	57.0 (50.0-63.7)	68.0 (54.2-79.2)
Positive predictive value (%)	45.2 (37.5-53.0)	37.7 (27.2-49.5)	33.8 (26.3-42.3)	52.9 (36.7-68.5)
Negative predictive value (%)	74.2 (66.7-80.4)	65.1 (58.9-70.8)	63.3 (56.1-70.0)	75.6 (61.3-85.7)
Accuracy (%)	59.7 (54.1-65.0)	59.0 (53.5-64.3)	50.1 (45.4-56.5)	65.8 (54.8-75.3)

Sociedade Brasileira de Genética Rua Cap. Adelmio Norberto da Silva, 736, 14025-670 Ribeirão Preto SP Brazil, Tel.: (55 16) 3911-4130 / Fax.: (55 16) 3621-3552 - Ribeirão Preto - SP - Brazil
E-mail: editor@gmb.org.br

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[1] Send correspondence to Claudia Lage. Laboratório de Radiações em Biologia, Carlos Chagas Filho Institute of Biophysics, CCS – Bldg G, Federal University of Rio de Janeiro (UFRJ) 21941-902 Rio de Janeiro, RJ, Brazil. E- mail: lage@biof.ufrj.br