Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region.

Elke M. Botzenhart; Gabriella Bartalini; Edward Blair; Angela F. Brady; Frances Elmslie; Karen L. Chong; Katie Christy; Wilfredo Torres-Martinez; Cesare Danesino; Matthew A. Deardorff; Jean Pierre Fryns; Sandrine Marlin; Sixto Garcia-Minaur; Yorck Hellenbroich; Beverly N. Hay; Maila Penttinen; Vandana Shashi; Paulien Terhal; Lionel Van Maldergem; Margo L. Whiteford; Elaine Zackai; Jürgen Kohlhase

doi:10.1002/humu.9476

Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region.

Elke M. Botzenhart^*, Gabriella Bartalini, Edward Blair, Angela F. Brady, Frances Elmslie, Karen L. Chong, Katie Christy, Wilfredo Torres-Martinez, Cesare Danesino, Matthew A. Deardorff, Jean Pierre Fryns, Sandrine Marlin, Sixto Garcia-Minaur, Yorck Hellenbroich, Beverly N. Hay, Maila Penttinen, Vandana Shashi, Paulien Terhal, Lionel Van Maldergem, Margo L. WhitefordElaine Zackai, Jürgen Kohlhase

^*Corresponding author for this work

Institute of Human Genetics

University of Freiburg

55 Citations (Scopus)

Abstract

Townes-Brocks syndrome (TBS) is an autosomal dominant malformation syndrome characterized by renal, anal, ear, and thumb anomalies caused by SALL1 mutations. To date, 36 SALL1 mutations have been described in TBS patients. All but three of those, namely p.R276X, p.S372X, and c.1404dupG, have been found only in single families thereby preventing phenotype-genotype correlations. Here we present 20 novel mutations (12 short deletions, five short duplications, three nonsense mutations) in 20 unrelated families. We delineate the phenotypes and report previously unknown ocular manifestations, i.e. congenital cataracts with unilateral microphthalmia. We show that 46 out of the now 56 SALL1 mutations are located between the coding regions for the glutamine-rich domain mediating SALL protein interactions and 65 bp 3' of the coding region for the first double zinc finger domain, narrowing the SALL1 mutational hotspot region to a stretch of 802 bp within exon 2. Of note, only two SALL1 mutations would result in truncated proteins without the glutamine-rich domain, one of which is reported here. The latter is associated with anal, ear, hand, and renal manifestations, indicating that the glutamine-rich domain is not required for typical TBS. (c) 2006 Wiley-Liss, Inc.

Original language	English
Journal	Human Mutation
Volume	28
Issue number	2
Pages (from-to)	204-205
Number of pages	2
ISSN	1059-7794
DOIs	https://doi.org/10.1002/humu.9476
Publication status	Published - 02.2007

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10.1002/humu.9476

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Botzenhart, E. M., Bartalini, G., Blair, E., Brady, A. F., Elmslie, F., Chong, K. L., Christy, K., Torres-Martinez, W., Danesino, C., Deardorff, M. A., Fryns, J. P., Marlin, S., Garcia-Minaur, S., Hellenbroich, Y., Hay, B. N., Penttinen, M., Shashi, V., Terhal, P., Van Maldergem, L., ... Kohlhase, J. (2007). Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region. Human Mutation, 28(2), 204-205. https://doi.org/10.1002/humu.9476

@article{466466b609914866b7b7fd9a7dcfb075,

title = "Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region.",

abstract = "Townes-Brocks syndrome (TBS) is an autosomal dominant malformation syndrome characterized by renal, anal, ear, and thumb anomalies caused by SALL1 mutations. To date, 36 SALL1 mutations have been described in TBS patients. All but three of those, namely p.R276X, p.S372X, and c.1404dupG, have been found only in single families thereby preventing phenotype-genotype correlations. Here we present 20 novel mutations (12 short deletions, five short duplications, three nonsense mutations) in 20 unrelated families. We delineate the phenotypes and report previously unknown ocular manifestations, i.e. congenital cataracts with unilateral microphthalmia. We show that 46 out of the now 56 SALL1 mutations are located between the coding regions for the glutamine-rich domain mediating SALL protein interactions and 65 bp 3' of the coding region for the first double zinc finger domain, narrowing the SALL1 mutational hotspot region to a stretch of 802 bp within exon 2. Of note, only two SALL1 mutations would result in truncated proteins without the glutamine-rich domain, one of which is reported here. The latter is associated with anal, ear, hand, and renal manifestations, indicating that the glutamine-rich domain is not required for typical TBS. (c) 2006 Wiley-Liss, Inc.",

author = "Botzenhart, \{Elke M.\} and Gabriella Bartalini and Edward Blair and Brady, \{Angela F.\} and Frances Elmslie and Chong, \{Karen L.\} and Katie Christy and Wilfredo Torres-Martinez and Cesare Danesino and Deardorff, \{Matthew A.\} and Fryns, \{Jean Pierre\} and Sandrine Marlin and Sixto Garcia-Minaur and Yorck Hellenbroich and Hay, \{Beverly N.\} and Maila Penttinen and Vandana Shashi and Paulien Terhal and \{Van Maldergem\}, Lionel and Whiteford, \{Margo L.\} and Elaine Zackai and J{\"u}rgen Kohlhase",

year = "2007",

month = feb,

doi = "10.1002/humu.9476",

language = "English",

volume = "28",

pages = "204--205",

journal = "Human Mutation",

issn = "1059-7794",

publisher = "John Wiley and Sons Inc",

number = "2",

}

Botzenhart, EM, Bartalini, G, Blair, E, Brady, AF, Elmslie, F, Chong, KL, Christy, K, Torres-Martinez, W, Danesino, C, Deardorff, MA, Fryns, JP, Marlin, S, Garcia-Minaur, S, Hellenbroich, Y, Hay, BN, Penttinen, M, Shashi, V, Terhal, P, Van Maldergem, L, Whiteford, ML, Zackai, E & Kohlhase, J 2007, 'Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region.', Human Mutation, vol. 28, no. 2, pp. 204-205. https://doi.org/10.1002/humu.9476

TY - JOUR

T1 - Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region.

AU - Botzenhart, Elke M.

AU - Bartalini, Gabriella

AU - Blair, Edward

AU - Brady, Angela F.

AU - Elmslie, Frances

AU - Chong, Karen L.

AU - Christy, Katie

AU - Torres-Martinez, Wilfredo

AU - Danesino, Cesare

AU - Deardorff, Matthew A.

AU - Fryns, Jean Pierre

AU - Marlin, Sandrine

AU - Garcia-Minaur, Sixto

AU - Hellenbroich, Yorck

AU - Hay, Beverly N.

AU - Penttinen, Maila

AU - Shashi, Vandana

AU - Terhal, Paulien

AU - Van Maldergem, Lionel

AU - Whiteford, Margo L.

AU - Zackai, Elaine

AU - Kohlhase, Jürgen

PY - 2007/2

Y1 - 2007/2

N2 - Townes-Brocks syndrome (TBS) is an autosomal dominant malformation syndrome characterized by renal, anal, ear, and thumb anomalies caused by SALL1 mutations. To date, 36 SALL1 mutations have been described in TBS patients. All but three of those, namely p.R276X, p.S372X, and c.1404dupG, have been found only in single families thereby preventing phenotype-genotype correlations. Here we present 20 novel mutations (12 short deletions, five short duplications, three nonsense mutations) in 20 unrelated families. We delineate the phenotypes and report previously unknown ocular manifestations, i.e. congenital cataracts with unilateral microphthalmia. We show that 46 out of the now 56 SALL1 mutations are located between the coding regions for the glutamine-rich domain mediating SALL protein interactions and 65 bp 3' of the coding region for the first double zinc finger domain, narrowing the SALL1 mutational hotspot region to a stretch of 802 bp within exon 2. Of note, only two SALL1 mutations would result in truncated proteins without the glutamine-rich domain, one of which is reported here. The latter is associated with anal, ear, hand, and renal manifestations, indicating that the glutamine-rich domain is not required for typical TBS. (c) 2006 Wiley-Liss, Inc.

AB - Townes-Brocks syndrome (TBS) is an autosomal dominant malformation syndrome characterized by renal, anal, ear, and thumb anomalies caused by SALL1 mutations. To date, 36 SALL1 mutations have been described in TBS patients. All but three of those, namely p.R276X, p.S372X, and c.1404dupG, have been found only in single families thereby preventing phenotype-genotype correlations. Here we present 20 novel mutations (12 short deletions, five short duplications, three nonsense mutations) in 20 unrelated families. We delineate the phenotypes and report previously unknown ocular manifestations, i.e. congenital cataracts with unilateral microphthalmia. We show that 46 out of the now 56 SALL1 mutations are located between the coding regions for the glutamine-rich domain mediating SALL protein interactions and 65 bp 3' of the coding region for the first double zinc finger domain, narrowing the SALL1 mutational hotspot region to a stretch of 802 bp within exon 2. Of note, only two SALL1 mutations would result in truncated proteins without the glutamine-rich domain, one of which is reported here. The latter is associated with anal, ear, hand, and renal manifestations, indicating that the glutamine-rich domain is not required for typical TBS. (c) 2006 Wiley-Liss, Inc.

UR - https://www.scopus.com/pages/publications/33847727918

U2 - 10.1002/humu.9476

DO - 10.1002/humu.9476

M3 - Journal articles

C2 - 17221874

AN - SCOPUS:33847727918

SN - 1059-7794

VL - 28

SP - 204

EP - 205

JO - Human Mutation

JF - Human Mutation

IS - 2

ER -

Townes-Brocks syndrome: twenty novel SALL1 mutations in sporadic and familial cases and refinement of the SALL1 hot spot region.

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