Characterization of the Human NIPSNAP1 Gene from 22q12: a Member of a Novel Gene Family

Overview

Journal Gene

Specialty Molecular Biology

Date 1998 May 29

PMID 9661659

Citations 15

Authors

E Seroussi

H Q Pan

D Kedra

B A Roe

J P Dumanski

Affiliations

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Abstract

Rapid progress in sequencing of human and other genomes allows high-resolution analysis of their gene content on the basis of comparison between species. We have used a combined computer and biochemical approach to characterize 135 kb of human genomic sequence from 22q12 and discovered a new 10 exon gene, termed NIPSNAP1, located between the neurofibromatosis type 2 and the pK1.3 genes. The NIPSNAP1 gene spans 26 kb of genomic sequence and shows to large introns in the 5'-region. All exon-intron junctions contain the gt/ag consensus splice site. The putative promoter of the NIPSNAP1 gene is TATA-less and resides in a GC-rich island characteristic of housekeeping genes. The NIPSNAP1 mRNA is 2.1 kb, is expressed ubiquitously at variable levels, with the highest expression in liver, is terminated by an uncommon ATTAAA polyadenylation site, and is capable of encoding a 284-amino-acid protein. This NIPSNAP1 protein has a strong sequence similarity limited to the central portion of a hypothetical protein (acc. P34492) from chromosome III of C. elegans, in which the other portions resemble a 4-nitrophenylphosphatase domain and non-neuronal SNAP25-like protein. Thus, the NIPSNAP1 gene is a member of an evolutionarily well conserved, novel gene family with two members in human and mouse that have now been characterized, and one member in C. elegans. The second human gene, NIPSNAP2, is localized in the vicinity of marker D7S499 on chromosome 7. Although the function of the NIPSNAP protein family is unknown, clues about its role may reside in the co-expression of the C. elegans orthologue, within an operon encoding protein motifs known to be involved in vesicular transport.

Citing Articles

Nipsnap1-A regulatory factor required for long-term maintenance of non-shivering thermogenesis.

Liu Y, Qu Y, Cheng C, Tsai P, Edwards K, Xue S Mol Metab. 2023; 75:101770.

PMID: 37423391 PMC: 10404556. DOI: 10.1016/j.molmet.2023.101770.

NIPSNAP1 directs dual mechanisms to restrain senescence in cancer cells.

Gao E, Sun X, Thorne R, Zhang X, Li J, Shao F J Transl Med. 2023; 21(1):401.

PMID: 37340421 PMC: 10280965. DOI: 10.1186/s12967-023-04232-1.

GBAS Regulates the Proliferation and Metastasis of Ovarian Cancer Cells by Combining with eEF1A1.

Ning X, Shi G, Ren S, Liu S, Ding J, Zhang R Oncologist. 2022; 27(1):e64-e75.

PMID: 35305106 PMC: 8842331. DOI: 10.1093/oncolo/oyab015.

Knockdown of GBAS regulates esophageal cancer cell viability and apoptosis.

Peng J, Ma K, Rong H, Xiao B, Zhu J, He J Mol Med Rep. 2021; 24(1).

PMID: 34036378 PMC: 8160481. DOI: 10.3892/mmr.2021.12162.

NIPSNAP protein family emerges as a sensor of mitochondrial health.

Fathi E, Yarbro J, Homayouni R Bioessays. 2021; 43(6):e2100014.

PMID: 33852167 PMC: 10577685. DOI: 10.1002/bies.202100014.