Gene Identification in 1.6-Mb Region of the Down Syndrome Region on Chromosome 21

Overview

Journal Genome Res

Specialty Genetics

Date 1997 Jan 1

PMID 9037601

Citations 17

Authors

M Ohira

N Seki

T Nagase

E Suzuki

N Nomura

O Ohara

M Hattori

Y Sakaki

T Eki

Y Murakami

T Saito

H Ichikawa

M Ohki

Affiliations

Soon will be listed here.

Abstract

The Down syndrome (DS) region has been defined by analyses of partial trisomy 21. The 2.5-Mb region between D21S17 and ERG is reportedly responsible for the main features of DS. Within this 2.5-Mb region, we focused previously on a distal 1.6-Mb region from an analysis of Japanese DS patients with partial trisomy 21. Previously we also performed exon-trapping and direct cDNA library screening of a fetal brain cDNA library and identified a novel gene TPRD. Further screening of a fetal heart cDNA library was performed and a total of 44 possible exons and 97 cDNA clones were obtained and mapped on a BamH1 map. By rescreening other cDNA libraries and a RACE reaction, we isolated nearly full-length cDNAs of three additional genes [holocarboxylase synthetase (HCS), G protein-coupled inward rectifier potassium channel 2 (GIRK2), and a human homolog of Drosophila minibrain gene (MNB)] and a coding sequence of a novel inward rectifier potassium channel-like gene (IRKK). The gene distribution and direction of transcription were determined by mapping both ends of the cDNA sequences. We found that these genes, except IRKK, are expressed ubiquitously and are relatively large, extending from 100 kb to 300 kb on the genome. These nearly full-length cDNA sequences should facilitate understanding of the detailed genome structure of the DS region and help to elucidate their role in the etiology of DS.

Citing Articles

Haploid-genetic screening of trophectoderm specification identifies as a repressor of totipotent-like status.

Zhang W, Sun S, Wang Q, Li X, Xu M, Li Q Sci Adv. 2023; 9(51):eadi5683.

PMID: 38117886 PMC: 10732524. DOI: 10.1126/sciadv.adi5683.

Insights from the protein interaction Universe of the multifunctional "Goldilocks" kinase DYRK1A.

Ananthapadmanabhan V, Shows K, Dickinson A, Litovchick L Front Cell Dev Biol. 2023; 11:1277537.

PMID: 37900285 PMC: 10600473. DOI: 10.3389/fcell.2023.1277537.

Dysregulation of ribosome-associated quality control elicits cognitive disorders via overaccumulation of TTC3.

Endo R, Chen Y, Burke J, Takashima N, Suryawanshi N, Hui K Proc Natl Acad Sci U S A. 2023; 120(12):e2211522120.

PMID: 36917672 PMC: 10041068. DOI: 10.1073/pnas.2211522120.

Histone acetylome-wide associations in immune cells from individuals with active Mycobacterium tuberculosis infection.

Del Rosario R, Poschmann J, Lim C, Cheng C, Kumar P, Riou C Nat Microbiol. 2022; 7(2):312-326.

PMID: 35102304 PMC: 9439955. DOI: 10.1038/s41564-021-01049-w.

GABA Receptors and Cognitive Processing in Health and Disease.

Vlachou S Curr Top Behav Neurosci. 2021; 52:291-329.

PMID: 34382179 DOI: 10.1007/7854_2021_231.