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Association between the ACE‑I/D polymorphism and nicotine dependence amongst patients with lung cancer (CROSBI ID 285329)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Nadalin, Sergej ; Flego, Veljko ; Dević Pavlić, Sanja ; Volarić, Darian ; Radojčić Badovinac, Anđelka ; Kapović, Miljenko ; Ristić, Smiljana Association between the ACE‑I/D polymorphism and nicotine dependence amongst patients with lung cancer // Biomedical reports, 13 (2020), 6; 58, 7. doi: 10.3892/br.2020.1365

Podaci o odgovornosti

Nadalin, Sergej ; Flego, Veljko ; Dević Pavlić, Sanja ; Volarić, Darian ; Radojčić Badovinac, Anđelka ; Kapović, Miljenko ; Ristić, Smiljana

engleski

Association between the ACE‑I/D polymorphism and nicotine dependence amongst patients with lung cancer

The biologically active peptide angiotensin II is cleaved from angiotensinogen by the renin and the angiotensin‑converting enzyme (ACE), an enzymatic cascade known as the renin‑angiotensin system (RAS). RAS may be important in the etiology of nicotine dependence by influencing dopaminergic signaling. In the present study, the association between an insertion/deletion (I/D) polymorphism of ACE and nicotine dependence amongst patients with lung cancer was assessed. To date, several studies have shown the relevance of this polymorphic variant in both nicotine dependence and lung cancer. However, the present study is the first to address the potential role of the ACE‑I/D polymorphism in nicotine dependence among patients with lung cancer. Genotyping was performed in 305 patients with lung cancer (males/females, 214/91). Significantly more male smokers had the ACE‑I allele compared with male non‑smokers (44.9 vs. 20.0% ; P<0.05). The risk of smoking was ~5‑fold higher for males with the ACE‑I allele (ACE‑II homozygous and ACE‑ID heterozygous) vs. ACE‑DD homozygous (odds ratio, 5.47 ; 95% confidence interval, 1.4‑21.9 ; P=0.016). The pack‑year smoking history in a subgroup of females with squamous cell carcinoma carrying the ACE‑I allele was significantly lower compared with ACE‑DD (37.1±14.1 vs. 57.0±29.1 ; F=4.5 ; P=0.046). The ACE‑I/D polymorphism accounted for 17.6% of the smoking severity in this patient group (β, ‑0.42 ; multiple R2 change, 0.176 ; P=0.046). These results suggest that the ACE‑I/D polymorphism contributes to the risk of nicotine dependence and smoking severity in lung cancer patients in a sex‑specific manner.

angiotensin‑converting enzyme gene ; insertion/deletion polymorphism ; lung cancer ; nicotine dependence

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Podaci o izdanju

13 (6)

2020.

58

7

objavljeno

2049-9434

2049-9442

10.3892/br.2020.1365

Povezanost rada

Biotehnologija u biomedicini (prirodno područje, biomedicina i zdravstvo, biotehničko područje)

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