Advanced search
Start date
Betweenand
Related content
(Reference retrieved automatically from Web of Science through information on FAPESP grant and its corresponding number as mentioned in the publication by the authors.)

Genetic control of renal tumorigenesis by the mouse Rtm1 locus

Full text
Author(s):
Show less -
Jensen, Jose Ricardo [1] ; Galvan, Antonella [2] ; Borrego, Andrea [1] ; Koury Cabrera, Wafa Hanna [1] ; Ribeiro, Orlando Garcia [1] ; Starobinas, Nancy [1] ; De Franco, Marcelo [1] ; Colecchia, Maurizio [3] ; Bertolotti, Alessia [3] ; Dragani, Tommaso Antonio [2] ; Martinez Ibanez, Olga Celia [1]
Total Authors: 11
Affiliation:
[1] Inst Butantan, Lab Immunogenet, BR-05503900 Sao Paulo - Brazil
[2] Fdn IRCCS Ist Nazl Tumori, Dept Predict & Prevent Med, Milan - Italy
[3] Fdn IRCCS Ist Nazl Tumori, Dept Pathol, Milan - Italy
Total Affiliations: 3
Document type: Journal article
Source: BMC Genomics; v. 14, OCT 22 2013.
Web of Science Citations: 6
Abstract

Background: The genetic basis of susceptibility to renal tumorigenesis has not yet been established in mouse strains. Mouse lines derived by bidirectional phenotypic selection on the basis of their maximal (AIRmax) or minimal (AIRmin) acute inflammatory responsiveness differ widely in susceptibility to spontaneous and urethane-induced renal tumorigenesis. To map the functional loci modulating renal tumor susceptibility in these mice, we carried out a genome-wide genetic linkage study, using SNP arrays, in an (AIRmax x AIRmin)F2 intercross population treated with a single urethane dose at 1 week of age and phenotyped for renal tumors at 35 weeks of age. Results: AIRmax mice did not develop renal tumors spontaneously nor in response to urethane, whereas in AIRmin mice renal tumors formed spontaneously (in 52% of animals) and after urethane induction (89%). The tumors had a papillary morphology and were positive for alpha-methylacyl-CoA racemase and negative for CD10. By analysis of 879 informative SNPs in 662 mice, we mapped a single quantitative trait locus modulating the incidence of renal tumors in the (AIRmax x AIRmin) F2 intercross population. This locus, which we named Renal tumor modifier QTL 1 (Rtm1), mapped to chromosome 17 at 23.4 Mb (LOD score = 15.8), with SNPs rs3696835 and rs3719497 flanking the LOD score peak. The A allele of rs3719497 from AIRmin mice was associated with a 2.5-fold increased odds ratio for renal tumor development. The LOD score peak included the Tuberous sclerosis 2 (Tsc2) gene which has already been implicated in kidney disease: loss of function by germline retroviral insertion is associated with spontaneous renal tumorigenesis in the Eker rat, and heterozygous-null Tsc2((+/-)) mice develop renal cystadenomas. Conclusions: We mapped Rtm1 as a single major locus modulating renal tumorigenesis in a murine intercross population. Thus, the AIR mouse lines can be considered a new genetic model for studying the role of germline and somatic molecular alterations in kidney neoplastic disease. (AU)

FAPESP's process: 11/21129-6 - Analysis of chromosomal regions which regulate susceptibility to inflammation and lung carcinogenesis in selected mouse lines
Grantee:Olga Celia Martinez Ibanez
Support Opportunities: Regular Research Grants