Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome.

Michael C Frühwald; Martin Hasselblatt; Sebastian Wirth; Gabriele Köhler; Reinhard Schneppenheim; Jose Igancio Martin Subero; Reiner Siebert; Uwe Kordes; Heribert Jürgens; Josef Vormoor

Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome.

Standard

Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome. / Frühwald, Michael C; Hasselblatt, Martin; Wirth, Sebastian; Köhler, Gabriele; Schneppenheim, Reinhard; Subero, Jose Igancio Martin; Siebert, Reiner; Kordes, Uwe; Jürgens, Heribert; Vormoor, Josef.

In: PEDIATR BLOOD CANCER, Vol. 47, No. 3, 3, 2006, p. 273-278.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Frühwald, MC, Hasselblatt, M, Wirth, S, Köhler, G, Schneppenheim, R, Subero, JIM, Siebert, R, Kordes, U, Jürgens, H & Vormoor, J 2006, 'Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome.', PEDIATR BLOOD CANCER, vol. 47, no. 3, 3, pp. 273-278. <http://www.ncbi.nlm.nih.gov/pubmed/16206192?dopt=Citation>

APA

Frühwald, M. C., Hasselblatt, M., Wirth, S., Köhler, G., Schneppenheim, R., Subero, J. I. M., Siebert, R., Kordes, U., Jürgens, H., & Vormoor, J. (2006). Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome. PEDIATR BLOOD CANCER, 47(3), 273-278. [3]. http://www.ncbi.nlm.nih.gov/pubmed/16206192?dopt=Citation

Vancouver

Frühwald MC, Hasselblatt M, Wirth S, Köhler G, Schneppenheim R, Subero JIM et al. Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome. PEDIATR BLOOD CANCER. 2006;47(3):273-278. 3.

Bibtex

@article{2b21d554755f4ecd9a6e86572d7d8e09,

title = "Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome.",

abstract = "BACKGROUND: Rhabdoid tumors represent an independent entity among embryonal neoplasms. These tumors affect the kidney (RTK, rhabdoid tumor of kidney) and central nervous system (AT/RT, atypical teratoid, rhabdoid tumor), but may also be found in peripheral soft tissue. Unifying features include immunohistochemical characteristics and inactivation of the putative tumor suppressor gene SMARCB1 (hSNF5/INI1) in chromosome 22q11.2. Several familial cases have been published and summarized under the term rhabdoid tumor predisposition syndrome. In all of the published familial cases, inactivation of SMARCB1 was detected in tumor tissues. PROCEDURE AND RESULTS: We report on a family with three children, two of which were affected by rhabdoid tumors, one RTK, the other an AT/RT. While both children demonstrated typical morphological and clinical features neither the RTK nor the AT/RT showed evidence for inactivation of SMARCB1 in molecular studies including CGH and array CGH, FISH, gene dosage analysis by dHPLC, and DNA-sequencing. Immunohistochemistry for SMARCB1 showed normal expression within the nuclei of tumor cells. Furthermore, both children inherited different paternal and maternal SMARCB1 alleles evidenced by haplotype analysis. Conventional cytogenetic, FISH, and mutation analyses lacked evidence for SMARCB1 aberrations or gross chromosomal changes in the parents. CONCLUSIONS: We thus demonstrate a family with rhabdoid tumor predisposition syndrome without linkage to SMARCB1. This finding indicates that other loci than SMARCB1 below the resolution of array CGH are involved in the origin of these tumors. Our data impact on the clinical counseling of affected families and warrant further studies in the molecular biology of these enigmatic tumors.",

author = "Fr{\"u}hwald, {Michael C} and Martin Hasselblatt and Sebastian Wirth and Gabriele K{\"o}hler and Reinhard Schneppenheim and Subero, {Jose Igancio Martin} and Reiner Siebert and Uwe Kordes and Heribert J{\"u}rgens and Josef Vormoor",

year = "2006",

language = "Deutsch",

volume = "47",

pages = "273--278",

journal = "PEDIATR BLOOD CANCER",

issn = "1545-5009",

publisher = "Wiley-Liss Inc.",

number = "3",

}

RIS

TY - JOUR

T1 - Non-linkage of familial rhabdoid tumors to SMARCB1 implies a second locus for the rhabdoid tumor predisposition syndrome.

AU - Frühwald, Michael C

AU - Hasselblatt, Martin

AU - Wirth, Sebastian

AU - Köhler, Gabriele

AU - Schneppenheim, Reinhard

AU - Subero, Jose Igancio Martin

AU - Siebert, Reiner

AU - Kordes, Uwe

AU - Jürgens, Heribert

AU - Vormoor, Josef

PY - 2006

Y1 - 2006

N2 - BACKGROUND: Rhabdoid tumors represent an independent entity among embryonal neoplasms. These tumors affect the kidney (RTK, rhabdoid tumor of kidney) and central nervous system (AT/RT, atypical teratoid, rhabdoid tumor), but may also be found in peripheral soft tissue. Unifying features include immunohistochemical characteristics and inactivation of the putative tumor suppressor gene SMARCB1 (hSNF5/INI1) in chromosome 22q11.2. Several familial cases have been published and summarized under the term rhabdoid tumor predisposition syndrome. In all of the published familial cases, inactivation of SMARCB1 was detected in tumor tissues. PROCEDURE AND RESULTS: We report on a family with three children, two of which were affected by rhabdoid tumors, one RTK, the other an AT/RT. While both children demonstrated typical morphological and clinical features neither the RTK nor the AT/RT showed evidence for inactivation of SMARCB1 in molecular studies including CGH and array CGH, FISH, gene dosage analysis by dHPLC, and DNA-sequencing. Immunohistochemistry for SMARCB1 showed normal expression within the nuclei of tumor cells. Furthermore, both children inherited different paternal and maternal SMARCB1 alleles evidenced by haplotype analysis. Conventional cytogenetic, FISH, and mutation analyses lacked evidence for SMARCB1 aberrations or gross chromosomal changes in the parents. CONCLUSIONS: We thus demonstrate a family with rhabdoid tumor predisposition syndrome without linkage to SMARCB1. This finding indicates that other loci than SMARCB1 below the resolution of array CGH are involved in the origin of these tumors. Our data impact on the clinical counseling of affected families and warrant further studies in the molecular biology of these enigmatic tumors.

AB - BACKGROUND: Rhabdoid tumors represent an independent entity among embryonal neoplasms. These tumors affect the kidney (RTK, rhabdoid tumor of kidney) and central nervous system (AT/RT, atypical teratoid, rhabdoid tumor), but may also be found in peripheral soft tissue. Unifying features include immunohistochemical characteristics and inactivation of the putative tumor suppressor gene SMARCB1 (hSNF5/INI1) in chromosome 22q11.2. Several familial cases have been published and summarized under the term rhabdoid tumor predisposition syndrome. In all of the published familial cases, inactivation of SMARCB1 was detected in tumor tissues. PROCEDURE AND RESULTS: We report on a family with three children, two of which were affected by rhabdoid tumors, one RTK, the other an AT/RT. While both children demonstrated typical morphological and clinical features neither the RTK nor the AT/RT showed evidence for inactivation of SMARCB1 in molecular studies including CGH and array CGH, FISH, gene dosage analysis by dHPLC, and DNA-sequencing. Immunohistochemistry for SMARCB1 showed normal expression within the nuclei of tumor cells. Furthermore, both children inherited different paternal and maternal SMARCB1 alleles evidenced by haplotype analysis. Conventional cytogenetic, FISH, and mutation analyses lacked evidence for SMARCB1 aberrations or gross chromosomal changes in the parents. CONCLUSIONS: We thus demonstrate a family with rhabdoid tumor predisposition syndrome without linkage to SMARCB1. This finding indicates that other loci than SMARCB1 below the resolution of array CGH are involved in the origin of these tumors. Our data impact on the clinical counseling of affected families and warrant further studies in the molecular biology of these enigmatic tumors.

M3 - SCORING: Zeitschriftenaufsatz

VL - 47

SP - 273

EP - 278

JO - PEDIATR BLOOD CANCER

JF - PEDIATR BLOOD CANCER

SN - 1545-5009

IS - 3

M1 - 3

ER -