Mucin-1

MUC1
	Gene ontology
Molecular function	protein binding; transcription coregulator activity; RNA polymerase II cis-regulatory region sequence-specific DNA binding; p53 binding;
Cellular component	extracellular region; cytoplasm; integral component of membrane; nucleus; Golgi lumen; integral component of plasma membrane; apical plasma membrane; membrane; vesicle; extracellular exosome; extracellular space; plasma membrane;
Biological process	positive regulation of histone H4 acetylation; regulation of transcription from RNA polymerase II promoter in response to stress; DNA damage response, signal transduction by p53 class mediator resulting in cell cycle arrest; negative regulation of intrinsic apoptotic signaling pathway in response to DNA damage by p53 class mediator; negative regulation of cell adhesion mediated by integrin; DNA damage response, signal transduction by p53 class mediator resulting in transcription of p21 class mediator; positive regulation of transcription from RNA polymerase II promoter in response to stress; O-glycan processing; negative regulation of transcription by competitive promoter binding; stimulatory C-type lectin receptor signaling pathway; cytokine-mediated signaling pathway;
	Sources:Amigo / QuickGO

Ensembl


ENSG00000185499


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UniProt


P15941 Q7Z551


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RefSeq (mRNA)

NM_001018016 NM_001018017 NM_001018021 NM_001044390 NM_001044391
NM_001044392 NM_001044393 NM_001204285 NM_001204286 NM_001204287 NM_001204288 NM_001204289 NM_001204290 NM_001204291 NM_001204292 NM_001204293 NM_001204294 NM_001204295 NM_001204296 NM_001204297 NM_002456 NM_182741 NM_001371720


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RefSeq (protein)

NP_001018016 NP_001018017 NP_001037855 NP_001037856 NP_001037857
NP_001037858 NP_001191214 NP_001191215 NP_001191216 NP_001191217 NP_001191218 NP_001191219 NP_001191220 NP_001191221 NP_001191222 NP_001191223 NP_001191224 NP_001191225 NP_001191226 NP_002447 NP_001358649 NP_001191217.1 NP_001191225.1 NP_001037856.1


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Location (UCSC)

Chr 1: 155.19 – 155.19 Mb

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PubMed search

^[2]

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Wikidata

View/Edit Human

Mucin-1 (MUC-1) is a heterodimer transmembrane protein of the mucin family encoded in humans by the MUC1 gene.^[3]^[4]^[5] It is cleaved into two chains: mucin-1 subunit alpha (MUC1-NT; MUC1-alpha) and mucin-1 subunit beta (MUC-CT; MUC1-beta). These subunits differ in size due to proteolytic cleavage of the translated precursor protein in the endoplasmic reticulum.^[6] The larger subunit of MUC-1 is characterized by numerous O-glycosylated bonds and a terminal sialic acid, creating a net negative charge on MUC-1.^[7] The smaller subunit contains a juxtamembrane region of the extracellular area, a transmembrane domain, and the cytoplasmic tail.^[7] The extracellular domain of MUC-1 is composed of 20 identical amino acid tandem repeats (TR).^[6] Each tandem repeat contains two serine and three threonine amino acid residues, providing five sites for potential O-glycosylation.^[6] MUC-1 protein is estimated to weigh 120 to 225 kDA.^[8]

The N-terminus of MUC-1 (MUC-1 N) contains variable number tandem repeats (VNTRs) of (PDTRPAPGSTAP PAHGVTSA). VNTR provides sites for glycosylation on proline, serine and threonine residues.^[9] The peptide backbone exhibits glycosidic bonds between serine and threonine within MUC-1 N. ^[10] Within the cytoplasmic tail of MUC-1, multiple phosphorylation sites exist due to the presence of threonine, tyrosine and serine amino acid residues.^[7] Alterations to the cytoplasmic tail may affect movement through the Golgi apparatus, thus affecting glycosylation of the tandem repeat domains of MUC-1.^[6] The C-terminus of MUC-1 (MUC-1 C) is short—the majority of weight comes from N-glycosylation.^[11] Research has shown that the C-terminus is linked to the development of inflammation and cancer.^[12]

MUC-1 is located in the apical membrane on simple epithelial cell surfaces. These cells are found in the human kidney, gallbladder, stomach, lung, pancreas, mammary gland, and the female reproductive tract.^[8] MUC-1 is removed from the membrane by endocytosis,^[13] internalized, re-glycosylated and recycled to the cell membrane.^[8]^[5]

Function

O-glycosylation and N-glycosylation in MUC-1 contribute to the formation of mucin.^[14] MUC-1 is a transcriptional coactivator involved in the activity and stabilization of enzymes and transcription of metabolic functions. MUC-1 regulates tyrosine kinase signaling receptors, which promote synthesis of biosynthetic intermediates used in cell growth.^[14] In normal cells, the tandem repeats and cytoplasmic tail of MUC-1 are significant in the regulation and progression of metastatic cancer. Alterations to these areas have shown a propensity of metastasis and progression in comparison to unaltered MUC-1 domains.^[6]

MUC-1 has many functions. MUC-1 is an inhibitor for cell-to-cell extracellular interactions for both normal and malignant cells.

stemness) in maintaining epithelial cell homeostasis.^[15]

In cancer

MUC-1 is over expressed in many forms of cancer.^[14] Given, MUC-1 is 10 times higher in cancer cells than normal cells,^[16] an over expression of MUC-1 in cancer can be indicative of aggressive, metastatic cancer, having a low response to therapy and survival rate.^[5] MUC-1 also exhibits altered glycosylation and aberrant surface distribution patterns in tumor cells.^[6] Tumor related MUC-1 disrupts and inhibits cell-cell and cell-matrix interactions and adherence.^[6] Inhibition of cellular interactions diminishes the adherence of immune effector cells to malignant cells, thereby creating an immunosuppressive effect.^[6] MUC-1 in cancerous epithelial cells exhibits a loss of polarity. This loss of polarity creates incomplete carbohydrate side chains, allowing the formation of new abnormal side chains, thus increasing tumorigenesis.^[10] In normal cells, MUC-1 is isolated to the apical surface of the cell. In cancer cells, over expression of MUC-1 is seen throughout the cell's nucleus, plasma membrane and cytoplasm.^[5] In addition to the membranous isoform, an alternatively spliced mucin-1 is secreted extracellularly.^[17]

MUC-1 in cancer is underglycosylated, causing interactions to form between MUC-1 core protein, transmembrane receptors, and extracellular components.^[8]^[5] The intercellular interaction between MUC-1 and the receptor ICAM-1 facilitates endothelial and epithelial cell interactions, allowing circulating cancer cells to adhere in the inner lining of blood vessels and thus migrate.^[5] MUC-1 over expression is controlled through transcription changes, post-translational, and amplification modifications. In transcription, MUC-1 in cancer is regulated through STAT proteins, hormones, hypoxia, and growth factors.^[5] MUC-1 plays a role in the increase of the autophagy of mitochondria, a process called mitophagy. An increase in mitophagy triggers the development and progression of cancer.^[15]

Breast cancer

MUC-1 is shown to be over expressed in 90% of

epithelial-mesenchymal transition, chromatin remodeling and epigenetic programming, which allow the cancer cells to avoid DNA damage and immune evasion. MUC-1 allows triple-negative breast cancer stem cells to engage in linear plasticity, a transition from one pathway into another, thus supporting the progression of TNBC.^[18]

Ovarian cancer

MUC-1 is over expressed in over 90% of all epithelial ovarian cancer. Currently, MUC-1 CT is being used to create therapies for ovarian cancer. Targeting MUC-1 CT to reduce expression has potential to control late-stage epithelial ovarian cancer. Since MUC-1 C does not contain a kinase or enzymatic function, targeting the protein's catalytic site is rendered useless. Research looking at breast cancer and MUC-1 showed promise in peptide blocking and disrupting MUC-1 CT interactions with specific effectors, decreasing proliferation, migration and invasion of metastatic breast cancer in vitro and inhibiting tumor growth and reoccurrence in mouse models. The results show promise for epithelial ovarian cancer therapies.^[6]

Cancer therapy

Studies have shown MUC-1 over expression creates drug resistance during chemotherapy by altering glycolytic metabolism.^[12] Over expression of MUC-1 decreases the apoptotic response to DNA damage, and increases anti-apoptotic Bcl-XL and PI3K/Akt pathways.^[6] MUC-1 in tumor cells suppresses mitochondria from releasing apoptotic factors, creating resistance to genotoxic anticancer agents.^[6] Cancer therapies are being developed to specifically target MUC-1 proteins, including peptide-based therapies, MUC-1 antibodies/conjugates, and MUC-1 vaccinations.^[5] Peptide-based therapies develop peptides that target tumors and attack membranes with a cytotoxic effect. ^[19] Murine antibodies that are reactive with MUC-1 VNTR domain have been produced through immunization using milk fat globule membranes, isolated mucin preparations, and tumor cells. Developed MUC-1 monoclonal antibodies are used in diagnosis of cancer, and creation of target therapies.^[6]

References

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000185499 – Ensembl, May 2017
^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ "UniProt". www.uniprot.org. Retrieved 7 November 2022.
^ "MUC1 Gene - GeneCards | MUC1 Protein | MUC1 Antibody". www.genecards.org. Retrieved 7 November 2022.
^
PMID 23303343
.

^
S2CID 254384521
.

^
PMID 15358196
.

^
PMID 14711375
.

S2CID 252649766
.

^
PMID 34207342
.

PMID 24667139
.

^
PMID 34207342
.

PMID 10712502
.

^
PMID 24418575
.

^
PMID 36289190
.

PMID 33167508
.

S2CID 25997699
.

^
PMID 35897789
.

PMID 22725698
.

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Retrieved from "https://en.wikipedia.org/w/index.php?title=Mucin-1&oldid=1188132035"

[refGRCh38Ensembl-1] GRCh38: Ensembl release 89: ENSG00000185499 – Ensembl, May 2017

[2] "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[UniProt-3] "UniProt". www.uniprot.org. Retrieved 7 November 2022.

[genecards-4] "MUC1 Gene - GeneCards | MUC1 Protein | MUC1 Antibody". www.genecards.org. Retrieved 7 November 2022.

[:0-5] 
PMID 23303343
.

[:2-6] 
S2CID 254384521
.

[:1-7] 
PMID 15358196
.

[Brayman_2004-8] 
PMID 14711375
.

[9] S2CID 252649766
.

[Chen_2021-10] 
PMID 34207342
.

[11] PMID 24667139
.

[Chen_2021_2-12] 
PMID 34207342
.

[13] PMID 10712502
.

[Mehla_2014-14] 
PMID 24418575
.

[Li_2022-15] 
PMID 36289190
.

[16] PMID 33167508
.

[17] S2CID 25997699
.

[Yamashita_2022-18] 
PMID 35897789
.

[19] PMID 22725698
.

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