Computational analyses of the effect of novel amino acid clusters of human transglutaminase 2 on its structure and function

Thangaraju, Kiruphagaran; Király, Róbert; Mótyán, János András; Ambrus, Viktor; Fuxreiter, Mónika; Fésüs, László

doi:10.1007/s00726-016-2330-0

Cited by 5 publications

(9 citation statements)

References 34 publications

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“…Lane 1: sequence of human TGM2, Lane 2: damaging nsSNVs in human TGM2. Functional regions of human TGM2: Intrinsically disordered regions (dark red) [ 4 ], amino acid clusters in light blue [ 30 ], fibronectin binding sites (FN) (green) K30, R116, and H134 [ 31 ], GDP binding residues (orange) S171, K173, R476, R478, V479, R580, Y583 [ 32 ], catalytic residues (pink); non-canonical Ca 2+ -binding sites: S4: 149–159, S1: 228–236, S3A: 305–311, S3B: 326–333, S2A: 395–401, S5: 432–440, and S2B: 445–455 (underlined and bolded) [ 33 ]. Domains of human TGM2 are presented vertically: β sandwich (1–139), catalytic core (147–460), β-barrel 1 (472–583), and β-barrel 2 (584–687).…”

Section: Resultsmentioning

confidence: 99%

“…Damaging nsSNVs are not present at active site residues (W241, C277, H335, and D358) and at recently described novel amino acid clusters emerged in humans [ 30 ]. We have previously identified additional residues around the active site, which are crucial for transamidase (W278) or isopeptidase (W332) activity [ 29 ] and there are no damaging nsSNV at these sites either.…”

Section: Resultsmentioning

confidence: 99%

“…A PolyPhen damaging variant with decreased activity is p.Val542Phe located within the MOD CK1 phosphorylation site and MOD PLK site phosphorylated by polo like kinases. Another potentially damaging variant p.Pro612Thr with less transamidase, isopeptidase and GTP binding is near to an IDR (597–602) and a novel amino acid cluster PVA (613–615) [ 30 ]. The homozygous variant p.Asp671Asn is located in the C-terminal class 3 PDZ-binding motif.…”

Section: Resultsmentioning

confidence: 99%

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Genomic variants reveal differential evolutionary constraints on human transglutaminases and point towards unrecognized significance of transglutaminase 2

et al. 2017

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Transglutaminases (TGMs) catalyze Ca2+-dependent transamidation of proteins with specified roles in blood clotting (F13a) and in cornification (TGM1, TGM3). The ubiquitous TGM2 has well described enzymatic and non-enzymatic functions but in-spite of numerous studies its physiological function in humans has not been defined. We compared data on non-synonymous single nucleotide variations (nsSNVs) and loss-of-function variants on TGM1-7 and F13a from the Exome aggregation consortium dataset, and used computational and biochemical analysis to reveal the roles of damaging nsSNVs of TGM2. TGM2 and F13a display rarer damaging nsSNV sites than other TGMs and sequence of TGM2, F13a and TGM1 are evolutionary constrained. TGM2 nsSNVs are predicted to destabilize protein structure, influence Ca2+ and GTP regulation, and non-enzymatic interactions, but none coincide with conserved functional sites. We have experimentally characterized six TGM2 allelic variants detected so far in homozygous form, out of which only one, p.Arg222Gln, has decreased activities. Published exome sequencing data from various populations have not uncovered individuals with homozygous loss-of-function variants for TGM2, TGM3 and TGM7. Thus it can be concluded that human transglutaminases differ in harboring damaging variants and TGM2 is under purifying selection suggesting that it may have so far not revealed physiological functions.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Genomic variants reveal differential evolutionary constraints on human transglutaminases and point towards unrecognized significance of transglutaminase 2

et al. 2017

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“…The white rhombus represents mutation N333S in a subject with MODY [43,45]. Triangles and bars represent SNPs detected in functional regions: cyan, SNPs in FN-binding site; violet, SNPs in amino acids probably significant for human TGM2 activities as described by Thangaraju et al [37]; black, SNPs in epitopes interacting with coeliac antibodies; green, SNPs in Bcl-2 protein family motif; grey, SNPs in nuclear location signals; yellow, SNP in amino acid in non-proline cis peptide bonds; orange, SNPs in putative Ca 2+ -binding sites; red, SNPs in GDP-binding and GTPase sites; brilliant green, SNPs in peptide regions involved in recognition and activation by the α1 B -adrenergic receptor; brown, SNPs in domain for PLCδ1 recognition. (B) Effects of SNP on the variant phenotype from the web site (http://snpeffect.switchlab.org/menu).…”

Section: Selective Roles Of Tg2 In Different Cellular Locationsmentioning

confidence: 97%

“…Supplementary Table S1 also lists the SNPs involved in alterations at 'amino acid clusters' of TG2 that were recently investigated by Thangaraju et al [37]. These authors focused attention on short sequences of 3-4 amino acids differing in murine and human TG2, which could be engaged in functional activity or stability of the protein, in the interaction with other proteins and in target sites for post-translational modifications.…”

Section: Selective Roles Of Tg2 In Different Cellular Locationsmentioning

confidence: 99%

Spotlight on the transglutaminase 2 gene: a focus on genomic and transcriptional aspects

Bianchi

Beninati

Bergamini

2018

Biochemical Journal

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The type 2 isoenzyme is the most widely expressed transglutaminase in mammals displaying several intra- and extracellular activities depending on its location (protein modification, modulation of gene expression, membrane signalling and stabilization of cellular interactions with the extracellular matrix) in relation to cell death, survival and differentiation. In contrast with the appreciable knowledge about the regulation of the enzymatic activities, much less is known concerning its inducible expression, which is altered in inflammatory and neoplastic diseases. In this context, we first summarize the gene's basic features including single-nucleotide polymorphism characterization, epigenetic DNA methylation and identification of regulatory regions and of transcription factor-binding sites at the gene promoter, which could concur to direct gene expression. Further aspects related to alternative splicing events and to ncRNAs (microRNAs and lncRNAs) are involved in the modulation of its expression. Notably, this important gene displays transcriptional variants relevant for the protein's function with the occurrence of at least seven transcripts which support the synthesis of five isoforms with modified catalytic activities. The different expression of the TG2 (type 2 transglutaminase) variants might be useful for dictating the multiple biological features of the protein and their alterations in pathology, as well as from a therapeutic perspective.

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TGase-mediated cell membrane modification and targeted cell delivery to inflammatory endothelium

et al. 2021

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Computational analyses of the effect of novel amino acid clusters of human transglutaminase 2 on its structure and function

Cited by 5 publications

References 34 publications

Genomic variants reveal differential evolutionary constraints on human transglutaminases and point towards unrecognized significance of transglutaminase 2

Genomic variants reveal differential evolutionary constraints on human transglutaminases and point towards unrecognized significance of transglutaminase 2

Spotlight on the transglutaminase 2 gene: a focus on genomic and transcriptional aspects

TGase-mediated cell membrane modification and targeted cell delivery to inflammatory endothelium

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