Metabolism and DNA Adduct Formation of Tobacco-Specific N-Nitrosamines
Abstract
:1. Introduction
2. Human Exposure to Carcinogenic Tobacco-Specific N-Nitrosamines
3. Metabolism and DNA Adduct Formation of NNK and Its Metabolite, NNAL
3.1. Occurrence and Carcinogenicity
3.2. Metabolism
3.2.1. Metabolic Activation and Detoxification Pathways
3.2.2. Stereochemistry of NNAL and Its Glucuronides
3.2.3. Stereochemistry of Hydroxy Acid Formation
3.3. DNA Adducts Formed by NNK Metabolism
3.3.1. POB DNA Adducts
- (1)
- HPB-releasing DNA Adducts
Animal Data | |||||||
---|---|---|---|---|---|---|---|
Animal Species | Administration Pathway | Exposure Amount | Exposure Duration | Target Tissue DNA | HPB-Releasing Adducts a | Ref. | |
Female A/J mice | Single i.p. injection | 10 μmol/mouse [5-3H]NNK | 12–144 h | Lung | 8.4 pmol/μmol Gua @ 24 h time point | [79] | |
Male F344 rats | Once daily i.p. injection | 15–5000 μg/kg/day of [5-3H]NNK or [C3H3]NNK | 4 days | Liver | 18–3400 fmol/mg DNA | [77] | |
Lung | 58–2180 fmol/mg DNA | ||||||
Single s.c. injection | 2 μmol/rat [5-3H]NNK | 24 h | Liver | 0.67 ± 0.1 pmol/mg DNA | [75] | ||
Lung | Present | ||||||
Single s.c. injection | 0.81 mg/kg of [5-3H]NNK | 24 h | Liver | 2.1 ± 0.1 pmol/μmol Gua | [76] | ||
Lung | 1.6 pmol/μmol Gua | ||||||
In the drinking water | 5 ppm NNK | 10 weeks | Lung | 9 ± 3 (pmol/mg DNA) | [24] | ||
30 weeks | 9 ± 3 | ||||||
50 weeks | 6 ± 1 | ||||||
70 weeks | 5 ± 2 | ||||||
5 ppm (S)-NNAL | 10 weeks | Lung | 5 ± 3 (pmol/mg DNA) | ||||
30 weeks | 10 ± 5 | ||||||
50 weeks | 11 ± 3 | ||||||
70 weeks | 5 ± 1 | ||||||
5 ppm (R)-NNAL | 10 weeks | Lung | 1 ± 0 (pmol/mg DNA) | ||||
30 weeks | 1 ± 1 | ||||||
50 weeks | 2 ± 1 | ||||||
70 weeks | 1 ± 1 | ||||||
Female A/J mice | Single i.p. injection | 10 μmol/mouse [5-3H]NNN | 24 h | Liver | 22.6 (or 25.1) pmol/μmol Gua | [80] | |
11 μmol/mouse [5-3H]NNN | Lung | 5.6 pmol/μmol Gua | [79] | ||||
Male F344 rats | Single s.c. injection | 0.35 μmol/rat [5-3H]NNN | 24 h | Liver | 0.08 ± 0.1 pmol/mg DNA | [75] | |
Once daily i.p. injection | 0.407 μmol/rat [5-3H]NNN | 3 days | Liver | 0.54 pmol/mg DNA | [81] | ||
Lung | 0.50 | ||||||
Nasal mucosa | 0.02 | ||||||
Esophagus | <0.005 | ||||||
Kidney | <0.005 | ||||||
Human Data | |||||||
Sample source | Smoking status | Subject number | Tissues | HPB-releasing adducts | Note | Ref. | |
Autopsy samples | Smokers verified by blood nicotine and cotinine, and medical record if necessary | 9 | Tracheobronchus | 16 ± 18 fmol/mg DNA | [80] | ||
Peripheral lung tissues | 11 ± 16 | ||||||
Nonsmokers | 8 | Tracheobronchus | 0.9 ± 1.7 | Only 1 subject had significant HPB levels. | |||
Peripheral lung tissues | 0.9 ± 2.3 | ||||||
TobPRAC Biorepository | Smokers (>10 cigs/day for at least 1 year) verified by urinary NNN and NNAL. | 30 | Mouthwash oral cells | 12.0 ± 35.1 pmol/mg DNA | [82] | ||
Buccal cells | 45 ± 57 | ||||||
Nonsmokers | 15 | Mouthwash oral cells | 0.23 ± 0.43 | Only 3 subjects had significant HPB levels. | |||
Patients with HNSCC | Smokers (determined by lifetime tobacco use questionnaire) | 30 | Buccal cells | 8.19 ± 17.8 (median 1.51) pmol/mg DNA | [83] | ||
Patients without HNSCC | 35 | 4.53 ± 14.36 (median 0.23) | |||||
Patients with lung cancers | Self-reported smokers | 21 | Peripheral lung tissues | 404 ± 258 fmol/mg DNA | [84] | ||
Self-reported nonsmokers | 11 | 59 ± 56 | |||||
Tumor-free sudden death victims | Smokers (>15 ng cotinine/mL blood or >100 ng cotinine/mL urine) | 32 | Lung | 92 ± 148 fmol/mg DNA | Primarily road traffic accidents, suicide and sudden cardiac arrest. | [85] | |
29 | Mucosa of esophagus | 138 ± 208 | |||||
12 | Mucosa of cardia | 93.6 ± 91.9 | |||||
Nonsmokers verified by blood or urinary cotinine | 56 | Lung | 61 ± 66 | ||||
53 | Mucosa of esophagus | 131 ± 130 | |||||
18 | Mucosa of cardia | 117 ± 110 | |||||
Patients with or without upper gastrointestinal disorders | Self-reported smokers | 7 | Mucosal biopsies of the lower esophagus | 4.80 ± 3.57 pmol/mg DNA | One outlier of patient #55 with ulcerative gastritis was excluded due to its exceptionally high level of HPB-releasing adducts (36.98 pmol/mg DNA) | [86] | |
Self-reported nonsmokers | 7 | 2.86 ± 2.44 |
- (2)
- POB DNA Base Adducts
- (3)
- POB DNA Phosphate Adducts
3.3.2. PHB DNA Adducts
- (1)
- PHB DNA Base Adducts
- (2)
- PHB DNA Phosphate Adducts
3.3.3. Methyl DNA Adducts
- (1)
- Methyl DNA Base Adducts
- (2)
- Methyl DNA Phosphate Adducts
3.3.4. Formaldehyde-Derived DNA Adducts
3.3.5. Summary of DNA Adducts Formed by NNK Metabolism
3.4. Mutagenicity and Genotoxicity of POB and PHB DNA Adducts
3.5. NNK-Derived DNA Adduct Formation in Lung Carcinogenesis
3.6. Human DNA Adducts Related to NNK Metabolism
3.6.1. HPB-Releasing DNA Adducts in Human Tissues
3.6.2. Methyl Phosphate Adducts in Human Lung
4. Metabolism and DNA Adduct Formation of NNN
4.1. Occurrence and Carcinogenicity
4.2. Metabolism
4.2.1. NNN α-Hydroxylation
- (1)
- Overall Metabolic Profiles of NNN in Laboratory Animals
- (2)
- Preferential α-Hydroxylation of NNN in Target Tissues
- (3)
- Selectivity of α-Hydroxylation of NNN in Target Tissues
4.2.2. NNN β-Hydroxylation
4.2.3. NNN Detoxification Pathways
4.2.4. Other Possible Metabolic Pathways
4.2.5. Stereochemistry of NNN Metabolism
4.3. DNA Adducts Formed by NNN Metabolism
4.3.1. DNA Adducts Formed by NNN 2′-Hydroxylation
- (1)
- POB DNA Base Adducts Formed by NNN 2′-Hydroxylation
- (2)
- POB DNA Phosphate Adducts Formed by NNN 2′-Hydroxylation
4.3.2. DNA Adducts Formed by NNN 5′-Hydroxylation
- (1)
- DNA Base Adducts Formed by NNN 5′-Hydroxylation
- (2)
- DNA Phosphate Adducts Formed by NNN 5′-Hydroxylation
4.4. Mutagenicity and Genotoxicity of NNN-Specific DNA Adducts
5. Concluding Remarks
Supplementary Materials
Author Contributions
Funding
Acknowledgments
Conflicts of Interest
Abbreviations
5′-AcetoxyNNN | 5′-acetoxy-N′-nitrosonornicotine |
AGT | O6-alkylguanine-DNA alkyltransferease |
AKRs | aldo-keto reductases |
AMMN | acetoxymethylmethylnitrosamine |
dIno | 2′-deoxyinosine |
dUrd | 2′-deoxyuridine |
E. Coli | Escherichia coli |
HPB | 4-hydroxy-1-(3-pyridyl)-1-butanone |
11β-HSD1 | 11β-hydroxysteroid dehydrogenase type 1 |
IARC | International Agency for Research on Cancer |
i.p. | intraperitoneal |
i.v. | intravenous |
N2-POBb-dGuo | N2-(4-(3-pyridyl)-4-oxobut-2-yl)-2′-deoxyguanosine |
Py-Py-dI | 2-[2-(3-pyridyl)-N-pyrrolidinyl]-2′-deoxyinosine |
Py-Py-dN | 6-[2-(3-pyridyl)-N-pyrrolidinyl]-2′-deoxynebularine |
N2-Py-Py(OH)-dI | N2-[2-(3-pyridyl)-N-pyrrolidinyl-5-hydroxy]-2′-deoxyinosine |
N6-Py-Py(OH)-dN | N6-[2-(3-Pyridyl)-N-pyrrolidinyl-5-hydroxy]-2′-deoxynebularine |
N2-Py-THF-dGuo | N2-[5-(3-pyridyl)tetrahydrofuran-2-yl]-2′-deoxyguanosine |
N6-HPB-dAdo | N6-[4-hydroxy-1-(pyridine-3-yl)butyl]-2′-deoxyadenosine |
N6-OPB-dAdo | N6-[4-oxo-1-(pyridine-3-yl)butyl]-2′-deoxyadenosine |
N6,N6-DHB-dAdo | N6,N6-(2,3-dihydroxybutan-1,4-diyl)-2′-deoxyadenosine |
NAB | N′-nitrosoanabasine |
NADP | nicotinamide adenosine dinucleotide phosphate |
NAT | N′-nitrosoanatabine |
NER | nucleotide excision repair |
NHANES | National Health and Nutrition Examination Survey |
NNAL | 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanol |
NNALOAc | 4-(acetoxymethylnitrosamino)-1-(3-pyridyl)-1-butanol |
NNAL-N-Gluc | 4-(methylnitrosamino)-1-(3-pyridyl-N-β-D-glycopyranuronosyl)-1-butanolonium inner salt |
NNAL-O-Gluc | 4-(methylnitrosamino)-1-(3-pyridyl)-1-(O-β-D-glucopyranuronosyl)butane |
NNC | nitrosamide N′-nitrosonorcotinine |
NNK | 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone |
NNKOAc | 4-((acetoxymethyl)nitrosamino)-1-(3-pyridyl)-1-butanone |
NNN | N′-nitrosonornicotine |
OPB | 4-oxo-4-(pyridin-3-yl)butanal |
OPB diazonium ion | 4-oxo-1-(pyridine-3-yl)butyl diazonium ion |
PATH study | Population Assessment of Tobacco and Health study |
PHB | pyridylhydroxybutyl |
POB | pyridyloxobutyl |
pol κ | polymerase κ |
ppm | parts per million |
s.c. | subcutaneous |
S. typhinurium | Salmonella typhinurium |
TLS | translesion synthesis |
TSNAs | tobacco-specific N-nitrosamines |
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DNA Adduct | Mutation | Cell | Ref. |
---|---|---|---|
POB DNA adduct | |||
O6-POB-dGuo | G > A (~90%) and G > T (~2%) | E. coli | [117] |
G > A (90%); G > T (~3%); other more complex types | HEK293 | [118] | |
G > A (~75%) and G > T (~3%) | HEK293T | [119] | |
O2-POB-Thd | T > G (37%) and T > A (12%) | E. coli | [120] |
T > A (47%) | HEK293T | [121] | |
T > A (~15%) | HEK293T | [119] | |
O4-POB-Thd | T > C (~35%) | HEK293T | [119] |
B1p(POB)B2 | Not mutagenic | E. coli | [105] |
PHB DNA adduct | |||
O6-PHB-dGuo | G > A (~95%) | E. coli | [117] |
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Li, Y.; Hecht, S.S. Metabolism and DNA Adduct Formation of Tobacco-Specific N-Nitrosamines. Int. J. Mol. Sci. 2022, 23, 5109. https://doi.org/10.3390/ijms23095109
Li Y, Hecht SS. Metabolism and DNA Adduct Formation of Tobacco-Specific N-Nitrosamines. International Journal of Molecular Sciences. 2022; 23(9):5109. https://doi.org/10.3390/ijms23095109
Chicago/Turabian StyleLi, Yupeng, and Stephen S. Hecht. 2022. "Metabolism and DNA Adduct Formation of Tobacco-Specific N-Nitrosamines" International Journal of Molecular Sciences 23, no. 9: 5109. https://doi.org/10.3390/ijms23095109