Intrinsic Disorder in Human Proteins Encoded by Core Duplicon Gene Families

Bibber, Nathan W. Van; Haerle, Cornelia; Khalife, Roy; Dayhoff, Guy W.; Uversky, Vladimir N.

doi:10.1021/acs.jpcb.0c07676

Cited by 6 publications

(4 citation statements)

References 118 publications

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“…We previously developed a web-crawler style disorder predictor for internal usage that was implemented into a tool we refer to as Disorder Spider (DiSpi) in our previous studies, see for example, refs. [34][35][36][37][38][39] DiSpi works by first aggregating disorder profiles from six well-known disorder predictors: PONDR VLXT, 40 PONDR VL3, 41 PONDR VLS2B, 42 PONDR-FIT, 43 IUPred-Short, and IUPred-Long. 44 Then, a mean disorder profile (MDP) is computed along with the standard error.…”

Section: Introductionmentioning

confidence: 99%

“…However, with a few exceptions, 32,33 these servers are not designed with genome‐scale structural bioinformatics or comparative genomics/proteomics in mind. We previously developed a web‐crawler style disorder predictor for internal usage that was implemented into a tool we refer to as Disorder Spider (DiSpi) in our previous studies, see for example, refs 34–39 . DiSpi works by first aggregating disorder profiles from six well‐known disorder predictors: PONDR VLXT, 40 PONDR VL3, 41 PONDR VLS2B, 42 PONDR‐FIT, 43 IUPred‐Short, and IUPred‐Long 44 .…”

Section: Introductionmentioning

confidence: 99%

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Rapid prediction and analysis of protein intrinsic disorder

Dayhoff

Uversky

2022

Protein Science

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Protein intrinsic disorder is found in all kingdoms of life and is known to underpin numerous physiological and pathological processes. Computational methods play an important role in characterizing and identifying intrinsically disordered proteins and protein regions. Herein, we present a new high‐efficiency web‐based disorder predictor named Rapid Intrinsic Disorder Analysis Online (RIDAO) that is designed to facilitate the application of protein intrinsic disorder analysis in genome‐scale structural bioinformatics and comparative genomics/proteomics. RIDAO integrates six established disorder predictors into a single, unified platform that reproduces the results of individual predictors with near‐perfect fidelity. To demonstrate the potential applications, we construct a test set containing more than one million sequences from one hundred organisms comprising over 420 million residues. Using this test set, we compare the efficiency and accessibility (i.e., ease of use) of RIDAO to five well‐known and popular disorder predictors, namely: AUCpreD, IUPred3, metapredict V2, flDPnn, and SPOT‐Disorder2. We show that RIDAO yields per‐residue predictions at a rate two to six orders of magnitude greater than the other predictors and completely processes the test set in under an hour. RIDAO can be accessed free of charge at https://ridao.app.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Rapid prediction and analysis of protein intrinsic disorder

Dayhoff

Uversky

2022

Protein Science

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“…Remarkably, we identified 113 unreviewed proteins containing NPIP-specific FUPs, with 91 being related to NPIP family and 22 lacking known functions, presumably derived from, hitherto, uncharacterized and novel genes, strongly suggesting the expansion of NPIP family with 22 additional protein members (Table 2A). Given the critical contribution of nuclear pore complex abnormalities to neurodegenerative diseases (18), the 22, putative new NPIP (Nuclear Pore Complex-Interacting Protein) family members, may prove to play essential roles in Alzheimer’s and Huntington pathologies (17, 19).…”

Section: Resultsmentioning

confidence: 99%

Uniquome: Construction and Decoding of a Novel Proteomic Atlas that Contains New Peptide Entities

Kontopodis,

Pierros,

Vorgias

et al. 2024

Preprint

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Cellular and molecular uniqueness has recently gained eminent importance, due to the large amount of data produced by -omics technologies. Herein, we have constructed and decoded the 'Uniquome' by introduction of the new peptide entities: (a) 'Core Unique Peptide' (CrUP), defined as the peptide whose sequence is accommodated, specifically and exclusively, only in one protein in a given proteome, and also bears the minimum length of amino acid sequence; (b) 'Composite Unique Peptide' (CmUP), defined as the peptide composed by the linear unification of CrUPs, when two or more successive in order CrUPs overlap one another; (c) 'Family Unique Peptide' (FUP), defined as the CrUPs that are common between all members of a given family, but unique only for the protein members of the particular family, and (d) 'Universal Unique Peptides' (UUPs), which are the common CrUPs in a given protein across organisms, carrying the important ability to securely identify a protein independently of an organism. By these entities as a tool-box, we have analyzed the human and model organisms, respective, proteomes. We demonstrate that these novel peptide entities play a crucial role for protein identification, protein-function prediction, cell physiology, tissue pathology, therapeutic oncology and translational medicine. Finally, we suggest that across species the conserved sequences are not DNA nucleotides but CrUPs entities.

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“…This signature is potentially consistent with recent neofunctionalization and diversification of this gene family in humans. It is interesting that a recent analysis of the putative protein structure encoded by 10 of the core duplicons, including TBC1D3, are enriched for disordered regions that may enhance protein-protein interactions or post-translational modification (Bibber et al 2020).…”

Section: Discussionmentioning

confidence: 99%

Independent expansion, selection and hypervariability of theTBC1D3gene family in humans

Guitart,

Porubsky,

Yoo

et al. 2024

Preprint

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TBC1D3 is a primate-specific gene family that has expanded in the human lineage and has been implicated in neuronal progenitor proliferation and expansion of the frontal cortex. The gene family and its expression have been challenging to investigate because it is embedded in high identity and highly variable segmental duplications. We sequenced and assembled the gene family using long-read sequencing data from 34 humans and 11 nonhuman primate species. Our analysis shows that this particular gene family has independently duplicated in at least five primate lineages, and the duplicated loci are enriched at sites of large-scale chromosomal rearrangements on chromosome 17. We find that most humans vary along two TBC1D3 clusters where human haplotypes are highly variable in copy number, differing by as many as 20 copies, and structure (structural heterozygosity 90%). We also show evidence of positive selection, as well as a significant change in the predicted human TBC1D3 protein sequence. Lastly, we find that, despite multiple duplications, human TBC1D3 expression is limited to a subset of copies and, most notably, from a single paralog group: TBC1D3-CDKL. These observations may help explain why a gene potentially important in cortical development can be so variable in the human population.

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Intrinsic Disorder in Human Proteins Encoded by Core Duplicon Gene Families

Cited by 6 publications

References 118 publications

Rapid prediction and analysis of protein intrinsic disorder

Rapid prediction and analysis of protein intrinsic disorder

Uniquome: Construction and Decoding of a Novel Proteomic Atlas that Contains New Peptide Entities

Independent expansion, selection and hypervariability of theTBC1D3gene family in humans

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