Your search keyword '"Ishqi, Hassan Mubarak"' showing total 3 results

1. Identification and expression of alternatively spliced novel isoforms of cancer associated MYD88 lacking death domain in mouse

Author

Ishqi, Hassan Mubarak, Husain, Mohammed Amir, Rehman, Sayeed Ur, Sarwar, Tarique, and Tabish, Mohammad

Published

2018

2. Differentially expressed novel alternatively spliced transcript variant of tumor suppressor Stk11 gene in mouse.

Author

Ishqi, Hassan Mubarak, Sarwar, Tarique, Husain, Mohammed Amir, Rehman, Sayeed Ur, and Tabish, Mohammad

Subjects

*TUMOR suppressor proteins, *SERINE/THREONINE kinases, *C-terminal residues, *PHOSPHORYLATION, *GLYCOSYLATION

Abstract

Serine/threonine kinase 11 (STK11) is a protein kinase that is encoded by Stk11 gene located on chromosome 19 and 10 in humans and mouse respectively. It acts as a master kinase of adenine monophosphate-activated protein kinase (AMPK) pathway that coordinates the regulation of cellular energy metabolism and cell division. STK11 exerts effect by activating more than 14 kinases including AMPK and AMPK-related kinases. It is also known to regulate cell polarity and acts as tumor suppressor. Alternative splicing of pre-mRNA is a mechanism which results in multiple transcript variants of a single gene. In human, two STK11 isoforms have been reported, an alternatively spliced isoform which has variation at its C-terminal and mostly expressed in testis (LKB1 S ). Another isoform exhibiting oncogenic properties lacks few residues at its N-terminal (ΔN-LKB1). In the present study, we report the identification of a new transcript variant Stk11N which is generated through alternative splicing. The new variant was found to have differential and tissue specific expression at Postnatal-7 and adult stages of mouse. As compared to the known variant Stk11C, the conceptually translated amino acid sequences of the new variant differ from exon-E2 onwards. In silico post translational studies of the new and published variant show similarity in some of the properties while differ in properties like nuclear export signals, phosphorylation, glycosylation, etc. Thus, alternative splicing of Stk11 gene generating new variant with heterogeneous properties suggests for complex regulation of these variants in controlling the AMPK pathway and other functions. [ABSTRACT FROM AUTHOR]

Published

2018

3. Identification of differentially expressed three novel transcript variants of mouse ARNT gene.

Author

Ishqi, Hassan Mubarak, Ur Rehman, Sayeed, Sarwar, Tarique, Husain, Mohammed Amir, and Tabish, Mohammad

Subjects

*ALTERNATIVE RNA splicing, *TRANSCRIPTION factors, *GENE expression, *MESSENGER RNA, *MOLECULAR biology

Abstract

The aryl hydrocarbon receptor nuclear translocator (ARNT/HIF1-β) is an obligatory transcriptional partner of the aryl hydrocarbon receptor (AHR) and hypoxia-inducible factor-1α (HIF-1α). It has a basic helix-loop-helix domain that belongs to period-ARNT-single-minded (PAS) protein family. PAS proteins act as heterodimeric transcription factors with ARNT being master dimerization partner. The ARNT-HIF-1α complex is an important transcriptional regulator of the hypoxic response of the tumor cells. Previous studies have reported two transcript variants of the gene produced by alternative splicing in mouse. One transcript variant contains all 22 exons while the other variant lacks exon-E5. In our study, using combinatorial approach comprising bioinformatics tools and molecular biology techniques involving RT-PCR, semi-nested PCR, sequencing and qPCR, we have identified three novel transcript variants of Arnt gene in mouse. All three new transcripts arise as a result of alternative splicing of newly identified exons with exon-E2, replacing reported exon-E1. These transcripts encode for three protein isofoms having different N-termini. The expression of these transcripts was found to be different in different tissues of adult mice. In silico analysis of the upstream region of the new exons revealed three distinct promoter regions designated as PA, PB and PC present upstream of newly identified exons. These promoters possess potential signature sequences for common as well as different transcription factors suggesting complex regulation of Arnt gene. In silico post translational studies of the conceptually translated amino acid sequences of these transcripts show similarity in some of the properties while differ in others. The diversity at N-termini of protein isoforms suggests the possibility of forming different complexes in different tissues and may also be important for unique interactions with partner molecules. © 2015 IUBMB Life, 68(2):122-135, 2016 [ABSTRACT FROM AUTHOR]

Published

2016