MUC16: molecular analysis and its functional implications in benign and malignant conditions

Haridas, Dhanya; Ponnusamy, Moorthy P.; Chugh, Seema; Lakshmanan, Imayavaramban; Seshacharyulu, Parthasarathy; Batra, Surinder K.

doi:10.1096/fj.14-257352

Cited by 97 publications

(101 citation statements)

References 133 publications

(207 reference statements)

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“…The ectodomain has a massive (12,000 amino acid) O-glycosylated domain, a tandem repeat domain consisting of more than 60 repeats of 156 amino acids, and S perm-E nterokinase-A grin (SEA) domains (O'Brien et al 2001 ;Yin and Lloyd 2001 ;Gipson et al 2014 ). Indirect evidence for the occurrence of MUC16 splice variants has been suggested [discussed in Haridas et al ( 2014 )]; however, mRNA splice variants have not been rigorously identifi ed. Fragments of MUC16 released from the cell surface are the CA 125 antigens commonly used as a serum marker for certain cancers, notably ovarian and endometrial (Patsner and Yim 2013 ;Baser et al 2014 ;Felder et al 2014 ), as well as endometriosis (Spaczynski and Duleba 2003 ).…”

Section: Structurementioning

confidence: 99%

Transmembrane Mucin Expression and Function in Embryo Implantation and Placentation

Constantinou

Morgado

Carson

2015

Advances in Anatomy, Embryology and Cell Biology

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Transmembrane mucins (TMs) are extremely large, complex glycoproteins that line the apical surfaces of simple epithelia including those of the female reproductive tract. TMs provide a physical barrier consistent with their role as part of the innate immune system. This barrier function must be overcome in the context of embryo implantation to permit blastocyst attachment. Three major TMs have been identified in uterine epithelia of multiple species: MUC1, MUC4, and MUC16. MUC1 has been found in all species studied to date, whereas expression of MUC4 and MUC16 have been less well studied and may be species specific. The strategies for removing mucins to permit embryo attachment also vary in a species-specific way and include both hormonal suppression of TM gene expression and membrane clearance via cell surface proteases. Studies emerging from the cancer literature indicate that TMs can modulate a surprisingly wide variety of signal transduction processes. Furthermore, various cell surface proteins have been identified that bind either the oligosaccharide or protein motifs of TMs suggesting that these molecules may support cell attachment in some contexts, including trophoblast interactions with cells of the immune system. The intimate association of TMs at sites of embryo-maternal interaction and the varied functions these complex molecules can play make them key players in embryo implantation and placentation processes.

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Section: Structurementioning

confidence: 99%

Transmembrane Mucin Expression and Function in Embryo Implantation and Placentation

Constantinou

Morgado

Carson

2015

Advances in Anatomy, Embryology and Cell Biology

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“…MUC16 is believed to play important roles not only in normal contexts such as reproduction and proliferation, but also in pathologic states including cancer and mucosal infections. It exerts its function in cancer by many mechanisms such as migration, invasion, cell cycle control and metabolism reprogramming (16,17). Since its discovery, CA125 is usually used as a tumor marker, and many efforts have been given to its contribution to tumor malignancies, yet little is known about its regulation.…”

Section: Introductionmentioning

confidence: 99%

Oncogenic KRAS Targets MUC16/CA125 in Pancreatic Ductal Adenocarcinoma

Liang

Qin

Zhang

et al. 2017

Molecular Cancer Research

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“…It has a short transmembrane domain and cytoplasmic tail of 32 amino acids. (For review of MUC16 structure see Haridas et al (Haridas et al, 2014), and Govindarajan and Gipson (Govindarajan and Gipson, 2010)). An antibody, termed H185, specific to a glycan on MUC16 (Argueso et al, 2003) was found by immunoelectron microscopy to bind microplicae on the surface of human corneal and conjunctival epithelium, but the antibody was also found to bind to goblet cell mucin packets in human conjunctival epithelium obtained by impression cytology (Danjo et al, 1998).…”

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confidence: 99%

Human conjunctival goblet cells express the membrane associated mucin MUC16: Localization to mucin granules

Gipson

Spurr-Michaud

Tisdale

2016

Experimental Eye Research

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MUC16 is an extraordinarily large 22,152 amino acid membrane spanning mucin that has been shown to be present in the glycocalyx of the apical cells of the human cornea and conjunctiva where is interfaces with the tear film. The ectodomain of the molecule has been demonstrated in tears, where it has been presumed to be from surface epithelial cells. Data presented here from multiple assays, including immunohistochemistry, immunoelectron microscopy, in situ hybridization, and RT-PCR of RNA isolated from goblet cells isolated by laser capture microdissection, demonstrate that the membrane tethered mucin is also expressed by conjunctival goblet cells both in humans and in mice. The mucin is present in mucin granules and appears to be localized to the mucin granule membrane. Correlation analyses of the amounts of the goblet cell secreted mucin MUC5AC and the amounts of MUC16 and of MUC1 another membrane tethered mucin ectodomain found in human tear samples demonstrated that MUC5AC amounts correlated to the amounts of MUC16 but not to MUC1. These data suggest that goblet cells are a second source of the mucin in tears. The function of the membrane tethered mucin in the mucin granule remains to be determined.

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MUC16: molecular analysis and its functional implications in benign and malignant conditions

Cited by 97 publications

References 133 publications

Transmembrane Mucin Expression and Function in Embryo Implantation and Placentation

Transmembrane Mucin Expression and Function in Embryo Implantation and Placentation

Oncogenic KRAS Targets MUC16/CA125 in Pancreatic Ductal Adenocarcinoma

Human conjunctival goblet cells express the membrane associated mucin MUC16: Localization to mucin granules

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