Characterization of a 3;6 translocation associated with renal cell carcinoma

RE Foster; M Abdulrahman; Mark Morris; E Prigmore; S Gribble; B Ng; Dean Gentle; S Ready; PM Weston; MS Wiesener; T Kishida; M Yao; V Davison; JL Barbero; C Chu; NP Carter; Farida Latif; Eamonn Maher

doi:10.1002/gcc.20403

Characterization of a 3;6 translocation associated with renal cell carcinoma

RE Foster, M Abdulrahman, Mark Morris, E Prigmore, S Gribble, B Ng, Dean Gentle, S Ready, PM Weston, MS Wiesener, T Kishida, M Yao, V Davison, JL Barbero, C Chu, NP Carter, Farida Latif, Eamonn Maher

Birmingham Medical School

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24 Citations (Scopus)

Abstract

The most frequent cause of familial clear cell renal cell carcinoma (RCC) is von Hippel-Lindau disease and the VHL tumor suppressor gene (TSG) is inactivated in most sporadic clear cell RCC. Although there is relatively little information on the mechanisms of tumorigenesis of clear cell RCC without VHL inactivation, a subset of familial cases harbors a balanced constitutional chromosome 3 translocation. To date nine different chromosome 3 translocations have been associated with familial or multicentric clear cell RCC; and in three cases chromosome 6 was also involved. To identify candidate genes for renal tumorigenesis we characterized a constitutional translocation, t(3;6)(q22;q16.1) associated with multicentric RCC without evidence of VHL target gene dysregulation. Analysis of breakpoint sequences revealed a 1.3-kb deletion on chromosome 6 within the intron of a 2 exon predicted gene (NT_007299.434). However, RT-PCR analysis failed to detect the expression of this gene in lymphoblast, fibroblast, or kidney tumor cell lines. No known genes were disrupted by the translocation breakpoints but several candidate TSGs (e.g., EPHB1, EPHA7, PPP2R3A RNF184, and STAG1) map within close proximity to the breakpoints.

Original language	English
Pages (from-to)	311-317
Number of pages	7
Journal	Genes, Chromosomes and Cancer
Volume	46
Issue number	4
DOIs	https://doi.org/10.1002/gcc.20403
Publication status	Published - 1 Apr 2007

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Foster, RE., Abdulrahman, M., Morris, M., Prigmore, E., Gribble, S., Ng, B., Gentle, D., Ready, S., Weston, PM., Wiesener, MS., Kishida, T., Yao, M., Davison, V., Barbero, JL., Chu, C., Carter, NP., Latif, F., & Maher, E. (2007). Characterization of a 3;6 translocation associated with renal cell carcinoma. Genes, Chromosomes and Cancer, 46(4), 311-317. https://doi.org/10.1002/gcc.20403

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title = "Characterization of a 3;6 translocation associated with renal cell carcinoma",

abstract = "The most frequent cause of familial clear cell renal cell carcinoma (RCC) is von Hippel-Lindau disease and the VHL tumor suppressor gene (TSG) is inactivated in most sporadic clear cell RCC. Although there is relatively little information on the mechanisms of tumorigenesis of clear cell RCC without VHL inactivation, a subset of familial cases harbors a balanced constitutional chromosome 3 translocation. To date nine different chromosome 3 translocations have been associated with familial or multicentric clear cell RCC; and in three cases chromosome 6 was also involved. To identify candidate genes for renal tumorigenesis we characterized a constitutional translocation, t(3;6)(q22;q16.1) associated with multicentric RCC without evidence of VHL target gene dysregulation. Analysis of breakpoint sequences revealed a 1.3-kb deletion on chromosome 6 within the intron of a 2 exon predicted gene (NT_007299.434). However, RT-PCR analysis failed to detect the expression of this gene in lymphoblast, fibroblast, or kidney tumor cell lines. No known genes were disrupted by the translocation breakpoints but several candidate TSGs (e.g., EPHB1, EPHA7, PPP2R3A RNF184, and STAG1) map within close proximity to the breakpoints.",

author = "RE Foster and M Abdulrahman and Mark Morris and E Prigmore and S Gribble and B Ng and Dean Gentle and S Ready and PM Weston and MS Wiesener and T Kishida and M Yao and V Davison and JL Barbero and C Chu and NP Carter and Farida Latif and Eamonn Maher",

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doi = "10.1002/gcc.20403",

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Foster, RE, Abdulrahman, M, Morris, M, Prigmore, E, Gribble, S, Ng, B, Gentle, D, Ready, S, Weston, PM, Wiesener, MS, Kishida, T, Yao, M, Davison, V, Barbero, JL, Chu, C, Carter, NP, Latif, F & Maher, E 2007, 'Characterization of a 3;6 translocation associated with renal cell carcinoma', Genes, Chromosomes and Cancer, vol. 46, no. 4, pp. 311-317. https://doi.org/10.1002/gcc.20403

TY - JOUR

T1 - Characterization of a 3;6 translocation associated with renal cell carcinoma

AU - Foster, RE

AU - Abdulrahman, M

AU - Morris, Mark

AU - Prigmore, E

AU - Gribble, S

AU - Ng, B

AU - Gentle, Dean

AU - Ready, S

AU - Weston, PM

AU - Wiesener, MS

AU - Kishida, T

AU - Yao, M

AU - Davison, V

AU - Barbero, JL

AU - Chu, C

AU - Carter, NP

AU - Latif, Farida

AU - Maher, Eamonn

PY - 2007/4/1

Y1 - 2007/4/1

N2 - The most frequent cause of familial clear cell renal cell carcinoma (RCC) is von Hippel-Lindau disease and the VHL tumor suppressor gene (TSG) is inactivated in most sporadic clear cell RCC. Although there is relatively little information on the mechanisms of tumorigenesis of clear cell RCC without VHL inactivation, a subset of familial cases harbors a balanced constitutional chromosome 3 translocation. To date nine different chromosome 3 translocations have been associated with familial or multicentric clear cell RCC; and in three cases chromosome 6 was also involved. To identify candidate genes for renal tumorigenesis we characterized a constitutional translocation, t(3;6)(q22;q16.1) associated with multicentric RCC without evidence of VHL target gene dysregulation. Analysis of breakpoint sequences revealed a 1.3-kb deletion on chromosome 6 within the intron of a 2 exon predicted gene (NT_007299.434). However, RT-PCR analysis failed to detect the expression of this gene in lymphoblast, fibroblast, or kidney tumor cell lines. No known genes were disrupted by the translocation breakpoints but several candidate TSGs (e.g., EPHB1, EPHA7, PPP2R3A RNF184, and STAG1) map within close proximity to the breakpoints.

AB - The most frequent cause of familial clear cell renal cell carcinoma (RCC) is von Hippel-Lindau disease and the VHL tumor suppressor gene (TSG) is inactivated in most sporadic clear cell RCC. Although there is relatively little information on the mechanisms of tumorigenesis of clear cell RCC without VHL inactivation, a subset of familial cases harbors a balanced constitutional chromosome 3 translocation. To date nine different chromosome 3 translocations have been associated with familial or multicentric clear cell RCC; and in three cases chromosome 6 was also involved. To identify candidate genes for renal tumorigenesis we characterized a constitutional translocation, t(3;6)(q22;q16.1) associated with multicentric RCC without evidence of VHL target gene dysregulation. Analysis of breakpoint sequences revealed a 1.3-kb deletion on chromosome 6 within the intron of a 2 exon predicted gene (NT_007299.434). However, RT-PCR analysis failed to detect the expression of this gene in lymphoblast, fibroblast, or kidney tumor cell lines. No known genes were disrupted by the translocation breakpoints but several candidate TSGs (e.g., EPHB1, EPHA7, PPP2R3A RNF184, and STAG1) map within close proximity to the breakpoints.

U2 - 10.1002/gcc.20403

DO - 10.1002/gcc.20403

M3 - Article

C2 - 17205537

SN - 1045-2257

VL - 46

SP - 311

EP - 317

JO - Genes, Chromosomes and Cancer

JF - Genes, Chromosomes and Cancer

IS - 4

ER -

Characterization of a 3;6 translocation associated with renal cell carcinoma

Abstract

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