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TMEM101
Identifiers
Aliases	TMEM101, transmembrane protein 101
External IDs	MGI: 1923797; HomoloGene: 12649; GeneCards: TMEM101; OMA:TMEM101 - orthologs
Gene location (Human) Chr. Chromosome 17 (human)[1] Band 17q21.31 Start 44,011,188 bp[1] End 44,023,946 bp[1]
Gene location (Mouse) Chr. Chromosome 11 (mouse)[2] Band 11|11 D Start 102,043,372 bp[2] End 102,047,230 bp[2]
RNA expression pattern Bgee Human Mouse (ortholog) Top expressed in endometrium seminal vesicula body of pancreas mucosa of transverse colon tendon of biceps brachii muscle of thigh body of stomach stromal cell of endometrium right uterine tube buccal mucosa cell Top expressed in motor neuron cumulus cell medullary collecting duct renal corpuscle internal carotid artery external carotid artery lens fossa pineal gland primitive streak More reference expression data BioGPS n/a
Gene ontology Molecular function signal transducer activity Cellular component integral component of membrane membrane Biological process positive regulation of I-kappaB kinase/NF-kappaB signaling signal transduction Sources:Amigo / QuickGO
Orthologs Species Human Mouse Entrez 84336 76547 Ensembl ENSG00000091947 ENSMUSG00000020921 UniProt Q96IK0 Q91VP7 RefSeq (mRNA) NM_001304813 NM_001304814 NM_032376 NM_029649 RefSeq (protein) NP_001291742 NP_001291743 NP_115752 NP_083925 Location (UCSC) Chr 17: 44.01 – 44.02 Mb Chr 11: 102.04 – 102.05 Mb PubMed search [3] [4]
Wikidata
View/Edit Human View/Edit Mouse

Transmembrane protein 101 (TMEM101) is a protein that in humans is encoded by the TMEM101 gene.^[5] The TMEM101 protein has been demonstrated to activate the NF-κB signaling pathway.^[6] High levels of expression of TMEM101 have been linked to breast cancer.^[7]

Known aliases of TMEM101 include Putative NF-Kappa-B-Activating Protein 130, FLJ23987, and MGC4251.^[8]

TMEM101 is located on the minus strand of the long arm of human chromosome 17 at the locus 17q21.31.^[5] The gene is 12,758 bp long, and it ranges from position 44,011,188 to position 44,023,946 on chromosome 17.^[5] TMEM101 is located between the genes NAGS and LSM12.^[5]

NCBI RefSeq contains five mRNA transcript variants for TMEM101.^[5] Transcript variants 1, 2, and 3 have been found experimentally, while transcript variants X1 and X2 have been predicted computationally.^[5] The last three exons of all five transcript variants are identical. The second exon is identical in transcript variants X1, 2, X2, and 3. The first exon in each transcript variant differs in the 3' UTR.

There are two known isoforms of the TMEM101 protein. Isoform a is encoded by transcript variant 1, while isoform b is encoded by transcript variants 2 and 3.^[5] Transcript variants X1 and X2 are also predicted to encode isoform b. Isoform b lacks the first 58 amino acids following the N-terminus of isoform a, but the remaining 199 amino acids are identical to isoform a.

Isoform a of the TMEM101 protein has a predicted molecular weight of about 29 kDa and a theoretical isoelectric point of about 9.6.^[9] In terms of amino acid composition, TMEM101 is relatively rich in the hydrophobic amino acids leucine and tyrosine, and relatively poor in the hydrophilic amino acids asparagine and threonine.^[10] It is also relatively poor in the sum of the two negatively charged amino acids, aspartic acid and glutamic acid.^[10]

Isoform a of the TMEM101 protein contains 8 transmembrane domains.^[11]

The Ali2D, I-TASSER, and Phyre2 models all predict that the secondary structure of TMEM101 is predominately composed of alpha helices.^[12][13][14] The Phyre2 prediction is presented in the figure to the right.

The I-TASSER highest confidence model for the predicted tertiary structure for the TMEM101 protein resembles the structure of a polytopic transmembrane alpha-helical protein.^[13]

The lysine at position 4 in the TMEM101 protein is predicted to be acetylated by the EP300 acetyltransferase enzyme.^[15]

There are five predicted phosphorylation sites located outside of transmembrane domains on the cytoplasmic side of the TMEM101 protein, which are listed in the table below.^[16]

Immunofluorescent staining experiments have detected the TMEM101 protein in the plasma membrane and the nucleoplasm.^[17]

The Genomatix Gene2Promoter tool lists 7 promoter regions for the Homo sapiens TMEM101 gene.^[18] The promoter that is supported by the greatest number of mRNA transcripts is 1525 bp long and spans the base pairs 44014913-44016437 on the negative strand of human chromosome 17. This promoter overlaps the start of transcription of mRNA transcript variant 1.

The following table presents a selected list of transcription factors that are predicted by the Genomatix MatInspector tool to bind to the GXP_8985856 promoter.^[19]

According to RNA-Seq data, TMEM101 is expressed in a wide range of tissues with low tissue specificity.^[20] Relatively, it is expressed most highly in breast tissue, the seminal vesicles, the kidneys, and endometrial tissue.^[20]

A cross section of a mouse embryo that has been stained for TMEM101 mRNA using in situ hybridization techniques shows noticeably lower levels of TMEM101 transcript in the liver than in other tissues.^[21]

TMEM101 has been observed to be expressed at lower levels in ovarian endometriotic cells than in uterine endometrial cells within the same individuals.^[22][23]

TMEM101 has also been observed to be expressed at higher levels in estrogen receptor positive ovarian cancer tumors than in estrogen receptor negative ovarian cancer tumors in mouse xenograft models.^[24][25]

The IntAct database indicates that the following proteins that have been found to interact with the TMEM101 protein through two-hybrid screening experiments.^[26]

TMEM101 has orthologs in Mammalia, Sauropsida, Amphibia, Osteichthyes, Chondrichthyes, Mollusca, Annelida, Echinodermata, Cnidaria, and Placozoa, among others. A table of selected orthologs is listed below. There are no known paralogs of TMEM101.

The most distantly related species to humans that possesses an ortholog of TMEM101 is Trichoplax adhaerens. Given that Ctenophorans do not possess orthologs of TMEM101, it appears that TMEM101 originated in the basal ParaHoxozoa clade after its divergence from Ctenophora approximately 948 million years ago. Based on a molecular clock analysis, the protein sequence of TMEM101 has on average evolved faster than Cytochrome c but slower than Fibrinogen alpha.

TMEM101 cDNA transcripts have been demonstrated to activate the transcription of NF-κB controlled genes in human embryonic kidney cells.^[6]

TMEM101 has been noted as a biomarker of breast cancer. High expression of TMEM101 is associated with the Luminal molecular subtype of breast cancer.^[7] Additionally, high levels of TMEM101 are associated with an increased risk score for the diagnosis of early stage triple-negative breast cancer.^[27]