Glycoproteomic Analysis of Malignant Ovarian Cancer Ascites Fluid Identifies Unusual Glycopeptides

Miyamoto, Suzanne; Ruhaak, L. Renee; Stroble, Carol; Salemi, Michelle; Phinney, Brett S.; Lebrilla, Carlito B.; Leiserowitz, Gary S.

doi:10.1021/acs.jproteome.6b00548

Cited by 30 publications

(23 citation statements)

References 74 publications

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“…Furthermore, since IgG and IgA are among the most abundant glycosylated proteins in ascites fluid [23], N-glycans attached to these proteins are likely a source of the most abundant N-glycans being measured in total N-glycan analysis of OC ascites fluid as previously reported [24] . These results demonstrate our ability to identify N-glycans attached to some of the major sources of N-glycosylation (IgG and IgA) in OC ascites.…”

Section: Discussionmentioning

confidence: 99%

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Multiple Reaction Monitoring for the Quantitation of Serum Protein Glycosylation Profiles: Application to Ovarian Cancer

et al. 2017

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Ascites fluid is present in over 30% of diagnosed ovarian cancer (OC) cases and is produced when tumor cells metastasize into the peritoneal cavity. Because of increased interest in the immune status of ovarian cancer patients who present with metastatic ascites and the potential role that glycosylation plays with functions of the different immunoglobulins such as complement-dependent and antibody-dependent cytotoxicity largely through the activity of Fc receptors. Immunoglobulins IgA and IgG were affinity isolated from OC ascites fluids, N-glycans were released and analyzed while site specific glycan analyses of glycopeptides was performed using tandem MS/MS with nano-LC Chip/QTOF MS. Results revealed the heterogeneity of N-glycans present in each glycosylation site of IgA1, IgA2 and IgG. Interestingly, fucosylated glycans were present in certain sites while other sites contained no fucosylated glycans. Highly sialylated N-glycans were present in other IgA sites suggesting different functional roles for each specific site.

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Section: Discussionmentioning

confidence: 99%

“…Trypsin digestion was performed as previously described [12]. After trypsin digestion and clean-up (ZipTip, Omix C18 100 ml tips, Agilent, Santa Clara CA), peptides were lyophilized.…”

Section: Methodsmentioning

confidence: 99%

Multiple Reaction Monitoring for the Quantitation of Serum Protein Glycosylation Profiles: Application to Ovarian Cancer

et al. 2017

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“…EOC dissemination rarely follows an invasion-metastasis cascade where single cells or collective cell populations break through the basal lamina, penetrate surrounding tissues, and intravasate into the vasculature [26,27]. EOC can form loosely attached outgrowths that extend the apical boundary of the tissue mucosa [28].…”

Section: Eoc Peritoneal Disseminationmentioning

confidence: 99%

“…One of the characteristics of ascites-derived tumors is their high degree of cell-to-cell adhesion, cell surface deposition of ECM, and integrin activation [40,59,135]. Ascites contain soluble ECM [136,137], and EOC deposits ECM on cell surfaces [27,39,[59][60][61], suggesting that, in the suspended environment of a peritoneal cavity, EOC cells engage integrins to organize ECM adhesion and, thus, suppress cell death associated with anchorage deprivation (anoikis). ECM adhesion is required for growth factor-mediated signaling [138].…”

Section: Role Of Extracellular Matrixmentioning

confidence: 99%

Ovarian Cancer Dissemination—A Cell Biologist’s Perspective

Farsinejad

Cattabiani

Muranen

et al. 2019

Cancers

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Epithelial ovarian cancer (EOC) comprises multiple disease states representing a variety of distinct tumors that, irrespective of tissue of origin, genetic aberrations and pathological features, share common patterns of dissemination to the peritoneal cavity. EOC peritoneal dissemination is a stepwise process that includes the formation of malignant outgrowths that detach and establish widespread peritoneal metastases through adhesion to serosal membranes. The cell biology associated with outgrowth formation, detachment, and de novo adhesion is at the nexus of diverse genetic backgrounds that characterize the disease. Development of treatment for metastatic disease will require detailed characterization of cellular processes involved in each step of EOC peritoneal dissemination. This article offers a review of the literature that relates to the current stage of knowledge about distinct steps of EOC peritoneal dissemination, with emphasis on the cell biology aspects of the process.

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“…In malignant ascites also are an abundance of other biochemical components, including N, haptoglobin, fibronectin, lumican, fibulin, hemopexin, ceruloplasmin, alpha-1-antitrypsin, alpha-1-antichymotrypsin, and clusterin, hemopexin, and fibulin glycopeptides [89].…”

Section: Metabolic and Biochemical Parameters Of Communication Betweementioning

confidence: 99%

Ascitic Fluid in Ovarian Carcinoma – From Pathophysiology to the Treatment

Živadinović¹,

Petrić²,

Krtinić³

et al. 2017

Ascites - Physiopathology, Treatment, Complications and Prognosis

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Due to low symptomatology, a lack of screening, and relatively complicated diagnostic procedures of ovarian carcinoma, more and more women are believed to visit their doctors in advanced stage of the disease, complicated with ascitic fluid. There is an increasing evidence that peritoneal cytology is a subjective assessment with certain percentage of false-positive and false-negative results that may cause application of unnecessary chemotherapy or nonapplication of necessary chemotherapy. Maximal cytoreductive surgery followed by intraperitoneal or systemic chemotherapy remains to be the gold standard in preventing ascites. Ascites is not only a symptom of a disease, but a specific microenvironment for formation and mediation of protumorigenic signals that control ovarian cancer progression, proliferation, invasion, anti-apoptosis, chemoresistance and tumor heterogeneity. Acellular cytokines and immunological factors influence ovarian cancer progression and its ability to prevent immune responses of the body and tumor reaction to chemotherapy. Ascites contributes to disease dissemination, changing its course and final outcomes. Management of patients with ascites and ovarian carcinoma is complex and often the goal of the treatment is to target palliative procedures. Multidisciplinary approach is necessary in the management of these patients. Further investigations of new drugs and immunomodulators are needed aiming at prolonged periods between relapses.

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Glycoproteomic Analysis of Malignant Ovarian Cancer Ascites Fluid Identifies Unusual Glycopeptides

Cited by 30 publications

References 74 publications

Multiple Reaction Monitoring for the Quantitation of Serum Protein Glycosylation Profiles: Application to Ovarian Cancer

Multiple Reaction Monitoring for the Quantitation of Serum Protein Glycosylation Profiles: Application to Ovarian Cancer

Ovarian Cancer Dissemination—A Cell Biologist’s Perspective

Ascitic Fluid in Ovarian Carcinoma – From Pathophysiology to the Treatment

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