Localization of SMAD5 and its evaluation as a candidate myeloid tumor suppressor

Daniel P. Hejlik; Lazar V. Kottickal; Hong Liang; Jeff Fairman; Thaylon Davis; Teresa Janecki; David Sexton; William Perry; Sean V. Tavtigian; David H.F. Teng; Lalitha Nagarajan

Localization of SMAD5 and its evaluation as a candidate myeloid tumor suppressor

Daniel P. Hejlik, Lazar V. Kottickal, Hong Liang, Jeff Fairman, Thaylon Davis, Teresa Janecki, David Sexton, William Perry, Sean V. Tavtigian, David H.F. Teng, Lalitha Nagarajan

Genetics

Research output: Contribution to journal › Article › peer-review

26 Scopus citations

Abstract

Acquired interstitial or complete losses of chromosome 5 are recurring anomalies associated with preleukemic myelodysplasia and acute myelogenous leukemia with a poor prognosis. Previous studies have delineated a potential myeloid tumor suppressor locus to a <2.4-Mb interval between the genes for IL9 and EGR1 on 5q31. In this report, we have localized the SMAD5 gene, a homologue of the tumor suppressor genes SMAD4/DPC-4 and SMAD2/JV18.1, to the minimal myeloid tumor suppressor locus and characterized its open reading frame and genomic organization. SMAD5 transcripts are readily detectable in hematolymphoid tissues and leukemic blasts. Absence of intragenic mutations in the remaining SMAD5 allele of leukemic patients and multiple solid tumor cell lines prescreened for loss of heterozygosity suggests that SMAD5 may not be a common target of somatic inactivation in malignancy.

Original language	English (US)
Pages (from-to)	3779-3783
Number of pages	5
Journal	Cancer Research
Volume	57
Issue number	17
State	Published - Sep 1 1997

ASJC Scopus subject areas

Oncology
Cancer Research

Cite this

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title = "Localization of SMAD5 and its evaluation as a candidate myeloid tumor suppressor",

abstract = "Acquired interstitial or complete losses of chromosome 5 are recurring anomalies associated with preleukemic myelodysplasia and acute myelogenous leukemia with a poor prognosis. Previous studies have delineated a potential myeloid tumor suppressor locus to a <2.4-Mb interval between the genes for IL9 and EGR1 on 5q31. In this report, we have localized the SMAD5 gene, a homologue of the tumor suppressor genes SMAD4/DPC-4 and SMAD2/JV18.1, to the minimal myeloid tumor suppressor locus and characterized its open reading frame and genomic organization. SMAD5 transcripts are readily detectable in hematolymphoid tissues and leukemic blasts. Absence of intragenic mutations in the remaining SMAD5 allele of leukemic patients and multiple solid tumor cell lines prescreened for loss of heterozygosity suggests that SMAD5 may not be a common target of somatic inactivation in malignancy.",

author = "Hejlik, {Daniel P.} and Kottickal, {Lazar V.} and Hong Liang and Jeff Fairman and Thaylon Davis and Teresa Janecki and David Sexton and William Perry and Tavtigian, {Sean V.} and Teng, {David H.F.} and Lalitha Nagarajan",

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AU - Hejlik, Daniel P.

AU - Kottickal, Lazar V.

AU - Liang, Hong

AU - Fairman, Jeff

AU - Davis, Thaylon

AU - Janecki, Teresa

AU - Sexton, David

AU - Perry, William

AU - Tavtigian, Sean V.

AU - Teng, David H.F.

AU - Nagarajan, Lalitha

PY - 1997/9/1

Y1 - 1997/9/1

N2 - Acquired interstitial or complete losses of chromosome 5 are recurring anomalies associated with preleukemic myelodysplasia and acute myelogenous leukemia with a poor prognosis. Previous studies have delineated a potential myeloid tumor suppressor locus to a <2.4-Mb interval between the genes for IL9 and EGR1 on 5q31. In this report, we have localized the SMAD5 gene, a homologue of the tumor suppressor genes SMAD4/DPC-4 and SMAD2/JV18.1, to the minimal myeloid tumor suppressor locus and characterized its open reading frame and genomic organization. SMAD5 transcripts are readily detectable in hematolymphoid tissues and leukemic blasts. Absence of intragenic mutations in the remaining SMAD5 allele of leukemic patients and multiple solid tumor cell lines prescreened for loss of heterozygosity suggests that SMAD5 may not be a common target of somatic inactivation in malignancy.

AB - Acquired interstitial or complete losses of chromosome 5 are recurring anomalies associated with preleukemic myelodysplasia and acute myelogenous leukemia with a poor prognosis. Previous studies have delineated a potential myeloid tumor suppressor locus to a <2.4-Mb interval between the genes for IL9 and EGR1 on 5q31. In this report, we have localized the SMAD5 gene, a homologue of the tumor suppressor genes SMAD4/DPC-4 and SMAD2/JV18.1, to the minimal myeloid tumor suppressor locus and characterized its open reading frame and genomic organization. SMAD5 transcripts are readily detectable in hematolymphoid tissues and leukemic blasts. Absence of intragenic mutations in the remaining SMAD5 allele of leukemic patients and multiple solid tumor cell lines prescreened for loss of heterozygosity suggests that SMAD5 may not be a common target of somatic inactivation in malignancy.

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Localization of SMAD5 and its evaluation as a candidate myeloid tumor suppressor

Abstract

ASJC Scopus subject areas

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