The physical map of the human RET proto-oncogene

B Pasini; R M W Hofstra; L Yin; R Bocciardi; G Santamaria; P M Grootscholten; I Ceccherini; G Patrone; M Priolo; C H C M Buys; G Romeo

The physical map of the human RET proto-oncogene

B Pasini, R M W Hofstra, L Yin, R Bocciardi, G Santamaria, P M Grootscholten, I Ceccherini, G Patrone, M Priolo, C H C M Buys, G Romeo

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Abstract

The RET proto-oncogene, a transmembrane tyrosine kinase receptor, is involved in the development of at least five different disease phenotypes. RET is activated through somatic rearrangements in a number of cases of papillary thyroid carcinoma while germ-line point mutations are associated with three inherited cancer syndromes MEN 2A, MEN 2B and FMTC. Moreover, point mutations or heterozygous deletions of RET are found in the dominant form of Hirschsprung disease or congenital colonic aganglionosis. We cloned the entire RET genomic sequence in a contig of cosmids encompassing 150 kb, from the CA repeat sTCL-2 to the region upstream the RET promoter, and established the position of the 20 exons of the RET gene with respect to a detailed restriction map based on eight endonucleases. A new highly polymorphic CA repeat sequence was identified within intron 5 of RET (RET-INT5). Finally the orientation of RET on chromosome 10q11.2 made it possible to orientate three other genes rearranged with RET in papillary thyroid carcinomas, namely H4/D10S170 on 10q21, R1 alpha on 17q23 and RFG2/Ele1 on 10q11.2.

Original language	English
Pages (from-to)	1737-1743
Number of pages	7
Journal	Oncogene
Volume	11
Issue number	9
Publication status	Published - 2-Nov-1995

Keywords

RET PROTOONCOGENE
GENE STRUCTURE
MEN 2
HIRSCHSPRUNG DISEASE
CHROMOSOME 10
C-KIT GENE
TYROSINE KINASE
SEQUENCE SIMILARITY
PROTOONCOGENE RET
TRANSFORMING GENE
CDNA CLONING
CELL-LINE
LONG ARM
DNA
RECEPTOR

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title = "The physical map of the human RET proto-oncogene",

abstract = "The RET proto-oncogene, a transmembrane tyrosine kinase receptor, is involved in the development of at least five different disease phenotypes. RET is activated through somatic rearrangements in a number of cases of papillary thyroid carcinoma while germ-line point mutations are associated with three inherited cancer syndromes MEN 2A, MEN 2B and FMTC. Moreover, point mutations or heterozygous deletions of RET are found in the dominant form of Hirschsprung disease or congenital colonic aganglionosis. We cloned the entire RET genomic sequence in a contig of cosmids encompassing 150 kb, from the CA repeat sTCL-2 to the region upstream the RET promoter, and established the position of the 20 exons of the RET gene with respect to a detailed restriction map based on eight endonucleases. A new highly polymorphic CA repeat sequence was identified within intron 5 of RET (RET-INT5). Finally the orientation of RET on chromosome 10q11.2 made it possible to orientate three other genes rearranged with RET in papillary thyroid carcinomas, namely H4/D10S170 on 10q21, R1 alpha on 17q23 and RFG2/Ele1 on 10q11.2.",

keywords = "RET PROTOONCOGENE, GENE STRUCTURE, MEN 2, HIRSCHSPRUNG DISEASE, CHROMOSOME 10, C-KIT GENE, TYROSINE KINASE, SEQUENCE SIMILARITY, PROTOONCOGENE RET, TRANSFORMING GENE, CDNA CLONING, CELL-LINE, LONG ARM, DNA, RECEPTOR",

author = "B Pasini and Hofstra, {R M W} and L Yin and R Bocciardi and G Santamaria and Grootscholten, {P M} and I Ceccherini and G Patrone and M Priolo and Buys, {C H C M} and G Romeo",

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pages = "1737--1743",

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TY - JOUR

T1 - The physical map of the human RET proto-oncogene

AU - Pasini, B

AU - Hofstra, R M W

AU - Yin, L

AU - Bocciardi, R

AU - Santamaria, G

AU - Grootscholten, P M

AU - Ceccherini, I

AU - Patrone, G

AU - Priolo, M

AU - Buys, C H C M

AU - Romeo, G

PY - 1995/11/2

Y1 - 1995/11/2

N2 - The RET proto-oncogene, a transmembrane tyrosine kinase receptor, is involved in the development of at least five different disease phenotypes. RET is activated through somatic rearrangements in a number of cases of papillary thyroid carcinoma while germ-line point mutations are associated with three inherited cancer syndromes MEN 2A, MEN 2B and FMTC. Moreover, point mutations or heterozygous deletions of RET are found in the dominant form of Hirschsprung disease or congenital colonic aganglionosis. We cloned the entire RET genomic sequence in a contig of cosmids encompassing 150 kb, from the CA repeat sTCL-2 to the region upstream the RET promoter, and established the position of the 20 exons of the RET gene with respect to a detailed restriction map based on eight endonucleases. A new highly polymorphic CA repeat sequence was identified within intron 5 of RET (RET-INT5). Finally the orientation of RET on chromosome 10q11.2 made it possible to orientate three other genes rearranged with RET in papillary thyroid carcinomas, namely H4/D10S170 on 10q21, R1 alpha on 17q23 and RFG2/Ele1 on 10q11.2.

AB - The RET proto-oncogene, a transmembrane tyrosine kinase receptor, is involved in the development of at least five different disease phenotypes. RET is activated through somatic rearrangements in a number of cases of papillary thyroid carcinoma while germ-line point mutations are associated with three inherited cancer syndromes MEN 2A, MEN 2B and FMTC. Moreover, point mutations or heterozygous deletions of RET are found in the dominant form of Hirschsprung disease or congenital colonic aganglionosis. We cloned the entire RET genomic sequence in a contig of cosmids encompassing 150 kb, from the CA repeat sTCL-2 to the region upstream the RET promoter, and established the position of the 20 exons of the RET gene with respect to a detailed restriction map based on eight endonucleases. A new highly polymorphic CA repeat sequence was identified within intron 5 of RET (RET-INT5). Finally the orientation of RET on chromosome 10q11.2 made it possible to orientate three other genes rearranged with RET in papillary thyroid carcinomas, namely H4/D10S170 on 10q21, R1 alpha on 17q23 and RFG2/Ele1 on 10q11.2.

KW - RET PROTOONCOGENE

KW - GENE STRUCTURE

KW - MEN 2

KW - HIRSCHSPRUNG DISEASE

KW - CHROMOSOME 10

KW - C-KIT GENE

KW - TYROSINE KINASE

KW - SEQUENCE SIMILARITY

KW - PROTOONCOGENE RET

KW - TRANSFORMING GENE

KW - CDNA CLONING

KW - CELL-LINE

KW - LONG ARM

KW - DNA

KW - RECEPTOR

M3 - Article

SN - 0950-9232

VL - 11

SP - 1737

EP - 1743

JO - Oncogene

JF - Oncogene

IS - 9

ER -

The physical map of the human RET proto-oncogene

Abstract

Keywords

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