TMEM126A

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Identifiers
Aliases
External IDs	GeneCards: [1]
Orthologs
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	Wikidata
View/Edit Human

Transmembrane protein 126A is a mitochondrial transmembrane protein of unknown function coded for by the TMEM126A gene.^[1]^[2]

A nonsense mutation in the TMEM126A gene has been shown to be related to optic atrophy. TMEM126A shows higher levels of expression in the parathyroid gland^[3] as well as in the peripheral blood cells of Huntington's disease patients, indicating that expression of this protein has some relation to blood regulation.

TMEM126A has two isoforms and is found on the long arm of Chromosome 11 in region 1, band 4, sub-band 1.^[4] It is produced by the TMEM126 gene, which codes for a mRNA 726 base pairs long.^[5] which translates into a protein 195 amino acids long.^[6] In addition, this gene is expressed 1.8 times the average of a normal gene and has expression with the prostate, uterus, kidney, placenta, heart, brain, and a large number of other tissues.^[7]

Gene

Locus

TMEM126 is located on the long arm of chromosome 11 in humans. It is found on the first sub-band of the fourth band within the first region.^[5] This can be written as 11q14.1.

Aliases

TMEM126A is also known as OPA7 and DKFZp586c1924.

Homology/evolutionary history

TMEM126A has been highly conserved among mammals, never dropping below 60% sequence identity when aligned with the same protein sequence from other species. It has been less well conserved outside of mammals, although it is evident in both fish, birds, and some invertebrates.^[8]

Orthologs

	Genus and species	Common name	Date of divergence	Accession number	Sequence length	Sequence identity	Sequence similarity	Notes
1	Gorilla gorilla	Gorilla	8.8 mya	XP_004051968	195	98%	98%	Predicted
2	Pongo abelii	Sumatran orangutan	15.7 mya	NP_001127371.1	196	97%	98%	Three transmembrane regions
3	Macaca mulatta	Rhesus macaque	29.0 mya	NP_001248065	195	92%	95%
4	Bos Taurus	Cow	94.2 mya	NP_001032697	197	81%	87%	Three transmembrane regions
5	Canis lupus familiaris	Dog	94.2 mya	XP_850546	197	80%	87%	Predicted
6	Felis catus	Cat	94.2 mya	XP_003992716	197	78%	87%	Predicted
7	Sus scrofa	94.2 mya	NP_001230521	196	76%	86%
8	Mus musculus	Mouse	92.3 mya	NP_079736	196	71%	84%	Three transmembrane regions
9	Rattus norvegicus	Brown rat	92.3 mya	NP_001011557	196	70%	81%	Three transmembrane regions
10	Ornithorhynchus anatinus	Platypus	167.4 mya	XP_001514960	126	69%	82%
11	Sarcophilus harrisii	Tasmanian Devil	162.6 mya	XP_003764651	208	63%	80%	Predicted
12	Salmo salar	Atlantic salmon	400.1 mya	NP_001134999	206	47%	63%
13	Gallus gallus	Chicken	296.0 mya	XP_003640643	209	46%	70%	Low quality. Predicted.
14	Danio rerio	Zebra fish	400.1 mya	NP_957092	201	44%	67%
15	Xenopus laevis	African clawed frog	371.2 mya	NP_001079826	203	52%	69%
16	Cavia porcellus	Guinea pig	92.3 mya	XP_003468633	195	74%	83%
17	Ciona intestinalis	Vase tunicate	722.5 mya	XP_002124594	230	28%	46%

^[8]

Paralogs

TMEM126A has a single paralog: TMEM126B. It is also found at 11q14.1 and is also known as HT007.^[9] TMEM126B shares 36% sequence identity and 49% sequence similarity with TMEM126A.^[8] The central domain is conserved between TMEM126A and TMEM126B.^[10]

mRNA

Promoter Analysis

Promoter sequence:

TTCACCCAACACTGCTTCCAAATAAGCAGTACTCTGGAGAACACGAGAAATCCTCAGAAAAATAAGCTGCAGCTCTGAGG

TGCTGATTATGGTAGGGCAATCAATACAGATCAAAACATGGCACAGGGAGCTTAAGTTCCTAGGGAGAGTAGAAAATCGA

TAGAGCCAAGAAATAGCTCACCTTTGACTTATTTTTAACCTGAGTAGCTATCATATGCCAAGAGCTGTGCAGTTTTCATT

TACCCCATGCCAAGAACGTAAGTAGGCTCTACTGACCAGGAAGTTAAGTAATATGCCCGAGGTACGTTTTCAATGGAAGA

GGCTGACTGAGGGTCACCCAACTTATATCTCGAAATTTCACAATTTCTACAAGTTCTGTCCTGGGAGGCAAGAGTAGGTG

AAACGAGCACACTCTACGCCAGGCAAACAAACCTCAACGCTTAGCCTCCCGGCACCTCCTAGGGCCGGAAGCTTCTCAGC

CCAAAGCCGCTGCTGGCTGCAACCTCCGTCCCGCAGTCCAATTAGCAGCCGCGACCCGGCGCCCGCCCACGCCGCGTCAC

GAGTCAGCCAAAGATGGCTGCGCCCAGGTAATTTGAGCAAAGGCCACAGTGAACTCCGGCGTGGCTGAGGAAGGAGGAGG

CACCCACAGGCTGCTGGGAGGAGAGCATAAGGTACTGGTATTCCGGGGGAGGGGGTGAAGTAAATGTCCCGGTGTCAGGA

GAAGCACGACGCGG^[11]

Species	Max Identity
Gorilla gorilla	97%
Pan paniscus	96%
Pan troglodytes	95%
Papio anubis	92%
Pango abelii	92%
Macaca mullata	90%

^[8]

There was only one promoter sequence found by using ElDorado on Genomatix. It is 734 base pairs long and found far upstream of the coding region of TMEM126A. The promoter sequence experiences extremely high levels of expression among primates but could not be found in any other species.

mRNA Folding

The minimum free energy formation has a number of hairpin loops and bulges. Another formation exists with a much larger bulge but which maintains the same hairpin loops.

TMEM126A has a number of likely locations for the formation of hairpin loops, four of which are extremely likely.

Alternative Splicing

In some circumstances, the second exon of the TMEM126A mRNA can be spliced out. This exon contains the main starting codon for the gene. The loss of this region would delay the start of translation until the next methionine, which occurs later in exon 3. Ultimately, this causes a loss of a great deal of genetic information from exons 2 and three.

Protein

Isoforms

The protein has three isoforms (a,b and c). The first isoform is the main version and the longest while the other two are both shorter.

Secondary structure

TMEM126A has a mixture of alpha helices, beta strands and coils that make up its secondary structure. There are two regions of high alpha-helix density which correspond to the transmembrane regions of the protein.

Domains and motifs

TMEM126A contains four exons, two transmembrane regions, and three stem-loop capable regions.^[12]^[13]

Post-translational modifications

File:Hydrophobic sites for TMEM126A.jpg

Hydrophobic sites found on the transmembrane protein TMEM126A

A peptide interaction can be found at amino acid 82 and continues to amino acid 90. This regions has good solubility, thanks to the presence of both cysteine and valine, is not conserved in rabbits, which allows for antibody production, and demonstrates high hydrophobicity.

In addition, there are two glycosylation sites at amino acids 13 and 60.^[14] as well as one phosphorylation site at amino acid 40^[15]

Expression

TMEM126A is expressed ubiquitously throughout the human body at 1.8 times the normal expression level for human genes. It experiences especially high expression in the parathyroid gland.^[3] In addition, TMEM126A experiences higher levels of expression in peripheral blood cells in patients diagnosed with Huntington's disease as well as individuals who experience ocular dominance.

Interacting proteins

TMEM126A interacts with a number of proteins. MYC and MAX form a complex and promote transcription.^[16] There is interaction with ATP synthase and the optic atrophy protein.^[17] These interactions relate to the proteins function in the mitochondria as well as its medical applications.

Clinical significance

A nonsense mutation in the TMEM126A gene has been shown to be related to optic atrophy.^[18] This mutation occurs on the second exon of the protein. The mutation results in decreased expression of TMEM126A. It has been demonstrated that a mutated TMEM126A gene can be distinguished from a normal gene through the use of antibodies which recognize the differences between the two. Experiments have shown that it associates with CD137L in myeloid cells.^[19]

Model organisms

Model organisms have been used in the study of TMEM126A function. A conditional knockout mouse line called Tmem126a^{tm1a(EUCOMM)Wtsi} was generated at the Wellcome Trust Sanger Institute.^[20] Male and female animals underwent a standardized phenotypic screen^[21] to determine the effects of deletion.^[22]^[23]^[24]^[25] Additional screens performed: - In-depth immunological phenotyping^[26]

*Tmem126a* knockout mouse phenotype
Characteristic	Phenotype
All data available at.^[21]^[27]
Insulin	Normal
Homozygous viability at P14	Normal
Homozygous Fertility	Normal
Body weight	Normal
Neurological assessment	Normal
Grip strength	Normal
Dysmorphology	Normal
Indirect calorimetry	Normal
Glucose tolerance test	Normal
Auditory brainstem response	Normal
DEXA	Normal
Radiography	Normal
Eye morphology	Normal
Clinical chemistry	Normal
Haematology 16 Weeks	Normal
Peripheral blood leukocytes 16 Weeks	Normal
Heart weight	Normal
Salmonella infection	Normal
Spleen Immunophenotyping	Normal
Mesenteric Lymph Node Immunophenotyping	Normal
Epidermal Immune Composition	Abnormal
Influenza Challenge	Normal

References

↑ "Entrez Gene: transmembrane protein 126A".
↑ Wiemann S, Weil B, Wellenreuther R, Gassenhuber J, Glassl S, Ansorge W, Böcher M, Blöcker H, Bauersachs S, Blum H, Lauber J, Düsterhöft A, Beyer A, Köhrer K, Strack N, Mewes HW, Ottenwälder B, Obermaier B, Tampe J, Heubner D, Wambutt R, Korn B, Klein M, Poustka A (Mar 2001). "Toward a catalog of human genes and proteins: sequencing and analysis of 500 novel complete protein coding human cDNAs". Genome Research. 11 (3): 422–35. doi:10.1101/gr.GR1547R. PMC 311072. PMID 11230166.
↑ ^3.0 ^3.1 "EST Profile - Hs.533725".
↑ "Genecards: TMEM126A".
↑ ^5.0 ^5.1 "TMEM126A transmembrane protein 126A [Homo sapiens (human)] - Gene - NCBI".
↑ "transmembrane protein 126A".
↑ "AceView: TMEM126A".
↑ ^8.0 ^8.1 ^8.2 ^8.3 "BLAST: Basic Local Alignment Search Tool".
↑ "TMEM126B transmembrane protein 126B".
↑ Hanein S, Perrault I, Roche O, Gerber S, Khadom N, Rio M, Boddaert N, Jean-Pierre M, Brahimi N, Serre V, Chretien D, Delphin N, Fares-Taie L, Lachheb S, Rotig A, Meire F, Munnich A, Dufier JL, Kaplan J, Rozet JM (Apr 2009). "TMEM126A, encoding a mitochondrial protein, is mutated in autosomal-recessive nonsyndromic optic atrophy". American Journal of Human Genetics. 84 (4): 493–8. doi:10.1016/j.ajhg.2009.03.003. PMC 2667974. PMID 19327736.
↑ "ElDorado Introduction".
↑ "Homo sapiens transmembrane protein 126A (TMEM126A), RefSeqGene on chromosome 11". 2017-10-05.
↑ "transmembrane protein 126A isoform 1 [Homo sapiens]".
↑ "NetNGlyc 1.0 Server".
↑ "NetPhos 3.1 Server".
↑ "2 items (Homo sapiens) - STRING database".
↑ "STRING: Functional protein association networks".
↑ "Genecards: transmembrane protein 126A isoform 2".
↑ Bae JS, Choi JK, Moon JH, Kim EC, Croft M, Lee HW (Dec 2012). "Novel transmembrane protein 126A (TMEM126A) couples with CD137L reverse signals in myeloid cells". Cellular Signalling. 24 (12): 2227–36. doi:10.1016/j.cellsig.2012.07.021. PMC 3466360. PMID 22885069.
↑ Gerdin AK (2010). "The Sanger Mouse Genetics Programme: high throughput characterisation of knockout mice". Acta Ophthalmologica. 88: 925–7. doi:10.1111/j.1755-3768.2010.4142.x.
↑ ^21.0 ^21.1 "International Mouse Phenotyping Consortium".
↑ Skarnes WC, Rosen B, West AP, Koutsourakis M, Bushell W, Iyer V, Mujica AO, Thomas M, Harrow J, Cox T, Jackson D, Severin J, Biggs P, Fu J, Nefedov M, de Jong PJ, Stewart AF, Bradley A (Jun 2011). "A conditional knockout resource for the genome-wide study of mouse gene function". Nature. 474 (7351): 337–42. doi:10.1038/nature10163. PMC 3572410. PMID 21677750.
↑ Dolgin E (Jun 2011). "Mouse library set to be knockout". Nature. 474 (7351): 262–3. doi:10.1038/474262a. PMID 21677718.
↑ Collins FS, Rossant J, Wurst W (Jan 2007). "A mouse for all reasons". Cell. 128 (1): 9–13. doi:10.1016/j.cell.2006.12.018. PMID 17218247.
↑ White JK, Gerdin AK, Karp NA, Ryder E, Buljan M, Bussell JN, Salisbury J, Clare S, Ingham NJ, Podrini C, Houghton R, Estabel J, Bottomley JR, Melvin DG, Sunter D, Adams NC, Tannahill D, Logan DW, Macarthur DG, Flint J, Mahajan VB, Tsang SH, Smyth I, Watt FM, Skarnes WC, Dougan G, Adams DJ, Ramirez-Solis R, Bradley A, Steel KP (Jul 2013). "Genome-wide generation and systematic phenotyping of knockout mice reveals new roles for many genes". Cell. 154 (2): 452–64. doi:10.1016/j.cell.2013.06.022. PMC 3717207. PMID 23870131.
↑ "Infection and Immunity Immunophenotyping (3i) Consortium".
↑ "Infection and Immunity Immunophenotyping (3i) Consortium".

[entrez-1] "Entrez Gene: transmembrane protein 126A".

[pmid11230166-2] Wiemann S, Weil B, Wellenreuther R, Gassenhuber J, Glassl S, Ansorge W, Böcher M, Blöcker H, Bauersachs S, Blum H, Lauber J, Düsterhöft A, Beyer A, Köhrer K, Strack N, Mewes HW, Ottenwälder B, Obermaier B, Tampe J, Heubner D, Wambutt R, Korn B, Klein M, Poustka A (Mar 2001). "Toward a catalog of human genes and proteins: sequencing and analysis of 500 novel complete protein coding human cDNAs". Genome Research. 11 (3): 422–35. doi:10.1101/gr.GR1547R. PMC 311072. PMID 11230166.

[NCBI_EST_Profiles-3] 3.0 ^3.1 "EST Profile - Hs.533725".

[gene_cards-4] "Genecards: TMEM126A".

[TMEM126A_transmembrane_protein_126A-5] 5.0 ^5.1 "TMEM126A transmembrane protein 126A [Homo sapiens (human)] - Gene - NCBI".

[ncbi-6] "transmembrane protein 126A".

[aceview-7] "AceView: TMEM126A".

[NCBI_BLAST-8] 8.0 ^8.1 ^8.2 ^8.3 "BLAST: Basic Local Alignment Search Tool".

[TMEM126B_transmembrane_protein_126B-9] "TMEM126B transmembrane protein 126B".

[pmid19327736-10] Hanein S, Perrault I, Roche O, Gerber S, Khadom N, Rio M, Boddaert N, Jean-Pierre M, Brahimi N, Serre V, Chretien D, Delphin N, Fares-Taie L, Lachheb S, Rotig A, Meire F, Munnich A, Dufier JL, Kaplan J, Rozet JM (Apr 2009). "TMEM126A, encoding a mitochondrial protein, is mutated in autosomal-recessive nonsyndromic optic atrophy". American Journal of Human Genetics. 84 (4): 493–8. doi:10.1016/j.ajhg.2009.03.003. PMC 2667974. PMID 19327736.

[Genomatix:_El_Dorado-11] "ElDorado Introduction".

[12] "Homo sapiens transmembrane protein 126A (TMEM126A), RefSeqGene on chromosome 11". 2017-10-05.

[13] "transmembrane protein 126A isoform 1 [Homo sapiens]".

[NetNGlyc-14] "NetNGlyc 1.0 Server".

[NetPhos-15] "NetPhos 3.1 Server".

[MAX_[ENSP00000351490]-16] "2 items (Homo sapiens) - STRING database".

[17] "STRING: Functional protein association networks".

[ncbi_2-18] "Genecards: transmembrane protein 126A isoform 2".

[19] Bae JS, Choi JK, Moon JH, Kim EC, Croft M, Lee HW (Dec 2012). "Novel transmembrane protein 126A (TMEM126A) couples with CD137L reverse signals in myeloid cells". Cellular Signalling. 24 (12): 2227–36. doi:10.1016/j.cellsig.2012.07.021. PMC 3466360. PMID 22885069.

[mgp_reference-20] Gerdin AK (2010). "The Sanger Mouse Genetics Programme: high throughput characterisation of knockout mice". Acta Ophthalmologica. 88: 925–7. doi:10.1111/j.1755-3768.2010.4142.x.

[IMPCsearch_ref-21] 21.0 ^21.1 "International Mouse Phenotyping Consortium".

[pmid21677750-22] Skarnes WC, Rosen B, West AP, Koutsourakis M, Bushell W, Iyer V, Mujica AO, Thomas M, Harrow J, Cox T, Jackson D, Severin J, Biggs P, Fu J, Nefedov M, de Jong PJ, Stewart AF, Bradley A (Jun 2011). "A conditional knockout resource for the genome-wide study of mouse gene function". Nature. 474 (7351): 337–42. doi:10.1038/nature10163. PMC 3572410. PMID 21677750.

[mouse_library-23] Dolgin E (Jun 2011). "Mouse library set to be knockout". Nature. 474 (7351): 262–3. doi:10.1038/474262a. PMID 21677718.

[mouse_for_all_reasons-24] Collins FS, Rossant J, Wurst W (Jan 2007). "A mouse for all reasons". Cell. 128 (1): 9–13. doi:10.1016/j.cell.2006.12.018. PMID 17218247.

[pmid23870131-25] White JK, Gerdin AK, Karp NA, Ryder E, Buljan M, Bussell JN, Salisbury J, Clare S, Ingham NJ, Podrini C, Houghton R, Estabel J, Bottomley JR, Melvin DG, Sunter D, Adams NC, Tannahill D, Logan DW, Macarthur DG, Flint J, Mahajan VB, Tsang SH, Smyth I, Watt FM, Skarnes WC, Dougan G, Adams DJ, Ramirez-Solis R, Bradley A, Steel KP (Jul 2013). "Genome-wide generation and systematic phenotyping of knockout mice reveals new roles for many genes". Cell. 154 (2): 452–64. doi:10.1016/j.cell.2013.06.022. PMC 3717207. PMID 23870131.

[iii_ref-26] "Infection and Immunity Immunophenotyping (3i) Consortium".

[iii_ref_2-27] "Infection and Immunity Immunophenotyping (3i) Consortium".

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