p24/ING1-ALT1 and p47/ING1-ALT2, distinct alternative transcripts of p33/ING1

1 May 2000

journal article
research article
Published by Springer Nature in Journal of Human Genetics

Vol. 45 (3) , 177-181
https://doi.org/10.1007/s100380050206

Abstract

P33/ING1s (the growth inhibitor ING1 and candidate tumor suppressor ING1) are key players in the suppressive pathways for human tumorigenesis. We analyzed their complete transcripts, primary structures, and expression. The results led us to discover two novel and related alternatively spliced transcripts encoding p24/ING1-ALT1 and p47/ING1-ALT2. They share C-terminal residues with the candidate tumor suppressors p33/ING1. The candidate tumor suppressors p33/ING1 and p24/ING1-ALT1 were coexpressed in a variety of fetal and adult human tissues, but p47/ING1-ALT2 was minimally expressed.

Keywords

HUMAN GENETICS
CYTOGENETICS
MOLECULAR GENETICS
BIOCHEMICAL GENETICS
GENOMICS
POPULATION GENETICS
DEVELOPMENTAL GENETICS
CLINICAL GENETICS
HUMAN GENOME
PHARMACOGENETICS
STATISTICAL GENETICS
EPIGENETICS
GENETIC EPIDEMIOLOGY

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