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UBALD1

From Wikipedia, the free encyclopedia
UBALD1
Identifiers
AliasesUBALD1, FAM100A, PP11303, UBA like domain containing 1
External IDsMGI: 1916255; HomoloGene: 17055; GeneCards: UBALD1; OMA:UBALD1 - orthologs
Orthologs
SpeciesHumanMouse
Entrez
Ensembl
UniProt
RefSeq (mRNA)

NM_145253
NM_001330467

NM_145359

RefSeq (protein)

NP_001317396
NP_660296

NP_663334

Location (UCSC)n/aChr 16: 4.69 – 4.7 Mb
PubMed search[2][3]
Wikidata
View/Edit HumanView/Edit Mouse

UBALD1 (ubiquitin-associated like domain containing 1) is a protein encoded by the UBALD1 gene, located on chromosome 16 in humans.[4] UBALD1 has high ubiquitous tissue expression and localizes in the nucleus and cytoplasm. UBALD1 is conserved in animals, including invertebrates. An alias for UBALD1 is FAM100A.

Gene

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The human UBALD1 gene is located on the minus strand of chromosome 16 at cytogenetic location 16p13.3. The gene contains three exons and two introns, with a total gene length of 6,145 base pairs.[5]

Transcripts

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There are three isoforms of UBALD1 in humans, all of which contain three exons. UBALD1 isoform 1 has a mRNA sequence of 1,374 nucleotides and encodes the longest protein. Isoform 2 differs with an exclusion of 75 nucleotides at the start of exon 3, and isoform 3 differs with an insertion of 185 nucleotides at the end of exon 1.[4]

Human UBALD1 Isoforms
Human UBALD1 isoforms
Transcript Variant mRNA length Exon 1 length Exon 2 length Exon 3 length Protein Isoform Protein Length (AA)
1 (NM_145253.3) 1374 211 62 1099 1 (NP_660296.1) 177
2 (NM_001330467.2) 1299 211 62 1024 2 (NP_001317396.1) 152
3 (NM_001411032.1) 1559 396 62 1099 3 (NP_001397961.1) 122
Conceptual Translation of Human UBALD1

Protein

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Isoforms

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UBALD1 isoform 1 encodes the longest protein that consists of 177 amino acids. The protein sequence from isoform 2 is 85.9% identical to isoform 1. Isoform 2 contains an exclusion of 25 amino acids in exon 3 and lacks the PHA03247 domain. Isoform 3 greatly differs from isoform 1 and 2, being 35.6% identical to isoform 1. Isoform 3 contains 122 amino acids and an inclusion at exon 1, causing a frameshift of codons and earlier occurrence of its stop codon. Isoform 3 also lacks the PHA03247 domain.

Properties and domains

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The protein encoded by UBALD1 isoform 1 has a predicted isoelectric point of 6.13 and a molecular weight 19.0 kDa.[6][7] UBALD1 composition is rich in alanine and proline, and contains multiple duplets/triplets of these residues. Proline residues and multiplets are highly conserved, specifically within the PHA03247 domain. The protein contains one domain, PHA03247, or large tegument protein UL36 domain. Tegument protein UL36 is the largest tegument protein found in herpes simplex virus 1, and contains deubiquitinating activity.[8]

Structure

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Tertiary structure of human UBALD1

The UBALD1 protein secondary structure consists of mostly coils and four short alpha helical regions (positions 5-22, 25–46, 76–83, and 170–173).[9] Its tertiary structure is subsequently coiled and globular-like.

Regulation

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Gene Level Expression

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UBALD1 is a highly expressed gene, 1.4x more expressed than the average gene.[10] UBALD1 has ubiquitous expression, with its highest levels in the placenta, skeletal muscle, liver, and brain.[11] Within the brain, UBALD1 expression is highest in the hippocampal formation and olfactory regions[12]

UBALD1 protein schematic including PHA03247 tegument domain, nuclear export signals, and phosphorylation sites

Protein level regulation

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UBALD1 protein is predicted to localize in the nucleus and cytoplasm.[13] A nuclear export signal is located moderately at positions 79-85 and strongly at positions 174–177.[14] UBALD1 has many predicted phosphorylation and glycosylation sites, with known phosphorylation sites at S88, S90, S93, and S96.[15]

Evolutionary history

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Orthologs

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The ortholog space for UBALD1 is large, with its most distant orthologs diverging 694 million years ago in invertebrates. The orthologs include most vertebrates, such as mammals, birds, reptiles, amphibians, fishes, as well as some invertebrates, such as arthropods, cnidaria, mollusks, echinoderms, and nematodes. There are no orthologs in fungi, plants, or bacteria. Closely related orthologs, including mammals, birds, and reptiles, range 67-92% sequence similarity. Moderately related orthologs, including amphibians and fishes, range sequence 55-75% similarity. Distantly related orthologs, including invertebrates, range 29-50% sequence similarity.

UBALD1 Orthologs
Taxonomic Group Genus and species Common Name Date of Divergence (MYA) Sequence Length (AA) Sequence Similarity % Accession Number
Mammals Homo sapiens human 0 177 100 NP_660296.1
Mus musculus mouse 87 176 92.1 NP_663334.1
Phascolarctos cinereus koala 160 174 80.6 XP_020834285.1
Aves Gallus gallus chicken 319 162 76.3 XP_015150132.1
Strigops habroptila owl parrot 319 162 74.6 XP_030340656.1
Reptiles Chrysemys picta bellii painted turtle 319 165 76.3 XP_005312202.1
Varanus komodoensis komodo dragon 319 166 67.6 XP_044289341.1
Amphibians Geotrypetes seraphini gaboon caecilian 353 161 70.4 XP_033770542.1
Bufo bufo common toad 353 142 65.4 XP_040297017.1
Fishes Danio rerio zebra fish 431 155 68.0 NP_001002488.1
Petromyzon marinus sea lamprey 599 179 64.7 XP_032830618.1
Invertebrates Styela clava tunicates 603 111 42.9 XP_039256608.1
Strongylocentrotus purpuratus purple sea urchin 619 183 36.2 XP_785714.2
Trichoplax sp. H2 trichoplax 661 94 39.5 RDD43865.1
Vanessa tameamea kamehameha butterfly 694 151 50.5 XP_026499211.1
Gigantopelta aegis deep sea snail 694 128 42.1 XP_041363274.1
Mercenaria mercenaria hard clam 694 122 42.5 XP_045214261.1

Paralogs

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The human UBALD1 protein has one paralog, UBALD2, present in vertebrates but not invertebrates. They are similar, with a 63.1% sequence identity and 70.9% sequence similarity. UBALD2 protein has a length of 164 amino acids, predicted isoelectric point of 6.78 and molecular weight of 17.7 kDa. [7]

The UL36 tegument protein domain of UBALD1 is partially conserved in the UBALD2 paralog. UBALD1 has monoallelic expression, where as UBALD2 has biallelic expression.

Conservation

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Exon 1 and the beginning of exon 3 (positions 64–79), are highly conserved among strict and distant orthologs. Specifically, the proline residues in exon 3 (P65, P69, P72, P73, P76) are strongly conserved.

Interacting proteins

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UBALD1 has physical association with proteins MED8, found in the nucleus, and RPL9, found in the cytoplasm.[16] UBALD1 also associates with EPRS and EEF1E1, both of which are known to interact and be involved in the aminoacyl-tRNA synthetase multienzyme complex.[17]

Clinical Significance

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UBALD1 has been associated with various cancer types,[18] and was identified as a significantly elevated autoantibody in lymphoma patients.[19] Hypomethylation of the UBALD1 promoter region was associated with cell-cell adhesion, B cell activation, and lymphocyte activation, is a potential biomarker for predicting primary resistance to platinum-based chemotherapeutics.[20] UBALD1 hypomethylation is also associated with gender incongruence. UBALD1 has significant CpG hypomethylation in trans women assigned male at birth before receiving gender-affirming hormone therapy, compared to cis men assigned male at birth.[21]

References

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  1. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000039568Ensembl, May 2017
  2. ^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  3. ^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  4. ^ a b "UBALD1 UBA like domain containing 1 [Homo sapiens (Human)] - Gene - NCBI".
  5. ^ "UBALD1 Gene - GeneCards | UBAD1 Protein | UBAD1 Antibody".
  6. ^ "PhosphoSite".
  7. ^ a b https://web.expasy.org/compute_pi/
  8. ^ Schlieker, C., Korbel, G. A., Kattenhorn, L. M., & Ploegh, H. L. (2005). A deubiquitinating activity is conserved in the large tegument protein of the herpesviridae. Journal of virology, 79(24), 15582-15585.
  9. ^ Wei Zheng, Chengxin Zhang, Yang Li, Robin Pearce, Eric W. Bell, Yang Zhang. Folding non-homology proteins by coupling deep-learning contact maps with I-TASSER assembly simulations. Cell Reports Methods, 1: 100014 (2021).
  10. ^ "NCBI AceView".
  11. ^ "Gds3113 / 150432".
  12. ^ "Gene Detail :: Allen Brain Atlas: Mouse Brain".
  13. ^ Nakai, K. and Horton, P., PSORT: a program for detecting the sorting signals of proteins and predicting their subcellular localization, Trends Biochem. Sci, 24(1) 34-35 (1999).
  14. ^ "Services".
  15. ^ Hornbeck PV, Zhang B, Murray B, Kornhauser JM, Latham V, Skrzypek E PhosphoSitePlus, 2014: mutations, PTMs and recalibrations. Nucleic Acids Res. 2015 43:D512-20
  16. ^ Stelzl, U., Worm, U., Lalowski, M., Haenig, C., Brembeck, F. H., Goehler, H., ... & Wanker, E. E. (2005). A human protein-protein interaction network: a resource for annotating the proteome. Cell, 122(6), 957-968.
  17. ^ Szklarczyk D*, Gable AL*, Nastou KC, Lyon D, Kirsch R, Pyysalo S, Doncheva NT, Legeay M, Fang T, Bork P‡, Jensen LJ‡, von Mering C‡. The STRING database in 2021: customizable protein–protein networks, and functional characterization of user-uploaded gene/measurement sets . Nucleic Acids Res. 2021 Jan 8;49(D1):D605-12.PubMed
  18. ^ Chen, R., Mias, G. I., Li-Pook-Than, J., Jiang, L., Lam, H. Y., Chen, R., ... & Snyder, M. (2012). Personal omics profiling reveals dynamic molecular and medical phenotypes. Cell, 148(6), 1293-1307.
  19. ^ Tan, Q., Wang, D., Yang, J., Xing, P., Yang, S., Li, Y., ... & Shi, Y. (2020). Autoantibody profiling identifies predictive biomarkers of response to anti-PD1 therapy in cancer patients. Theranostics, 10(14), 6399.
  20. ^ Hua, T., Kang, S., Li, X. F., Tian, Y. J., & Li, Y. (2021). DNA methylome profiling identifies novel methylated genes in epithelial ovarian cancer patients with platinum resistance. Journal of Obstetrics and Gynaecology Research, 47(3), 1031-1039.
  21. ^ Ramirez, K., Fernández, R., Collet, S., Kiyar, M., Delgado-Zayas, E., Gómez-Gil, E., ... & Pásaro, E. (2021). Epigenetics is implicated in the basis of gender incongruence: an epigenome-wide association analysis. Frontiers in Neuroscience, 1074.