Esophageal
cancer is prevalent in Cixian, China, but the etiology
of this disease remains largely unknown. Therefore, we explored this
by conducting a DNA adductome analysis. Both tumorous and nontumorous
tissues were collected from patients who underwent surgical procedures
at Cixian Cancer Hospital and the Fourth Hospital of Hebei Medical
University, which is in a low-incidence area. N
2-(3,4,5,6-Tetrahydro-2H-pyran-2-yl)deoxyguanosine
(THP-dG) was the major adduct detected in samples from esophageal
cancer patients in Cixian. The precursor of THP-dG, N-nitrosopiperidine (NPIP), exhibited a strong mutagenic activity
under metabolic activation in the Ames test and a significant dose-dependent
increase in mutation frequency during an in vivo mutagenicity
test with guanine phosphoribosyltransferase (gpt)
delta rats. The NPIP-induced mutation was dominated by A:T to C:G
transversions, followed by G:C to A:T and A:T to G:C transitions,
in the liver and esophagus of animal samples. A similar mutational
pattern was observed in the mutational signature of esophageal cancer
patients that demonstrated weak correlation with THP-dG levels. These
findings suggested that NPIP exposure is partly involved in the development
of esophageal cancer in Cixian residents.
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