Effect of inactivating heterozygous mutations in DNA repair genes on experimental lung carcinogenesis in mice-Reference-Cited by-同舟云学术

Effect of inactivating heterozygous mutations in DNA repair genes on experimental lung carcinogenesis in mice

Published:2024-03-22 Issue:1 Volume:23 Page:37-44
ISSN:1726-9792
Container-title:Russian Journal of Biotherapy
language:
Short-container-title:Rossijskij bioterapevtičeskij žurnal

Author:

Maydin M. A.¹^ORCID,Yurova M. N.¹^ORCID,Fedoros E. I.¹^ORCID,Sergiev P. V.²^ORCID,Aleksakhina S. N.¹^ORCID,Otradnova E. A.¹^ORCID,Kruglov S. S.¹^ORCID,Imyanitov E. N.¹^ORCID

Affiliation:

1. N.N. Petrov National Medical Research Center of Oncology, Ministry of Health of Russia

2. M.V.Lomonosov Moscow State University

Abstract

Background. Inactivating mutations in Chek2 and Gprc5a genes are known to be associated with cancer development. Experimental carcinogenesis studies in genetically modified mice generate new data on their influence on pathology development.Aim. In the present study in a model of lung carcinogenesis, survival parameters as well as tumor multiplicity and size in mice with Chek2 and Gprc5a heterozygous inactivating mutations were evaluated.Material and methods. F2 hybrid mice from crosses between CBAB6F1 males heterozygous for the studied mutations and wild-type BALB / c females were used: Chek2dAA-carriers (76 males and 64 females) and Gprc5ainsA-carriers (60 males and 42 females). Starting at four months of age, mice received urethane (ethyl carbamate) intraperitoneally at a dose of 600 mg / kg weekly for 6 weeks. After genotyping by allele-specific PCR, animals were allocated to groups. Carcinogenesis parameters were evaluated 40 weeks after the beginning of the experiment.Results. The proportion of mice with mutations surviving to the age of three months roughly followed the Mendelian distribution (35 / 41 males and 33 / 31 females) for the offspring of males heterozygous for Chek2dAA and was significantly lower in the case of Gprc5ainsA (20 / 40 males and 17 / 25 females, p = 0.043). The death of Gprc5ainsA carriers during the experiment was also higher than in the control group (p = 0.0506 in females). Synchronous lung and thymus neoplasms were found in 2 out of 4 Gprc5ainsA females that died before the end of the experiment, which were not found in other groups. At the end of the experiment, no significant differences in tumor multiplicity, mean linear size, and volume were found between the groups of mice with and without mutations.Conclusion. It was found that heterozygous inactivating mutation Chek2dAA does not affect early age development and does not modify the parameters of induced lung carcinogenesis in mice. Heterozygous carriage of Gprc5ainsA mutation in mice increases the risk of early death and sensitivity to the toxic and carcinogenic effects of urethane.

Publisher

Publishing House ABV Press

Reference22 articles.

1. Imyanitov E.N., Byrski T. Systemic treatment for hereditary cancers: A 2012 update. Hered Cancer Clin Pract 2013;11(1):2. DOI: 10.1186/1897-4287-11-2

2. De Castro D.G., Clarke P.A., Al-Lazikani B., Workman P. Personalized cancer medicine: Molecular diagnostics, predictive biomarkers, and drug resistance. Clin Pharmacol Ther 2013;93(3):252–9. DOI: 10.1038/clpt.2012.237

3. Pritchard C.C., Mateo J., Walsh M.F. et al. Inherited DNA-repair gene mutations in men with metastatic prostate cancer. N Engl J Med 2016;375(5):443–53. DOI: 10.1056/NEJMOA1603144

4. Cybulski C., Górski B., Huzarski T. et al. CHEK2 is a multiorgan cancer susceptibility gene. Am J Hum Genet 2004;75(6):1131–5. DOI: 10.1086/426403

5. Kilpivaara O., Vahteristo P., Falck J. et al. CHEK2 variant I157T may be associated with increased breast cancer risk. Int J Cancer 2004;111(4):543–7. DOI: 10.1002/IJC.20299