Ceramide galactosyltransferase (UGT8) as a molecular marker of canine mammary tumor malignancy

Nowak, Marcin; Dzięgiel, Piotr; Madej, Janusz A.; Ugorski, Maciej

doi:10.5603/fhc.2013.0024

Cited by 8 publications

(5 citation statements)

References 18 publications

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“…UGT8 expression was shown to be upregulated in breast (610,806), ovarian (416), and lung (613) cancer. Moreover, breast cancer cell lines with a luminal epitheliallike phenotype expressed little or no UGT8, while malignant, more mesenchymal-like cells expressed relatively high levels (157,526). Immunohistochemical analyses showed that increased UGT8 expression correlated with increasing breast tumor grade; the same finding was also reported for canine mammary tumors (526).…”

Section: Ugt8 Outside Of the Nervous System: Kidney Testis Bone Marrow And Cancer Cellssupporting

confidence: 63%

“…Moreover, breast cancer cell lines with a luminal epitheliallike phenotype expressed little or no UGT8, while malignant, more mesenchymal-like cells expressed relatively high levels (157,526). Immunohistochemical analyses showed that increased UGT8 expression correlated with increasing breast tumor grade; the same finding was also reported for canine mammary tumors (526). Recently, UGT8 was listed as part of a six-gene predictive signature for breast cancer metastasis to lung (380).…”

Section: Ugt8 Outside Of the Nervous System: Kidney Testis Bone Marrow And Cancer Cellsmentioning

confidence: 53%

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The UDP-Glycosyltransferase (UGT) Superfamily: New Members, New Functions, and Novel Paradigms

Meech

McKinnon

et al. 2019

Physiological Reviews

193

128

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UDP-glycosyltransferases (UGTs) catalyze the covalent addition of sugars to a broad range of lipophilic molecules. This biotransformation plays a critical role in elimination of a broad range of exogenous chemicals and by-products of endogenous metabolism, and also controls the levels and distribution of many endogenous signaling molecules. In mammals, the superfamily comprises four families: UGT1, UGT2, UGT3, and UGT8. UGT1 and UGT2 enzymes have important roles in pharmacology and toxicology including contributing to interindividual differences in drug disposition as well as to cancer risk. These UGTs are highly expressed in organs of detoxification (e.g., liver, kidney, intestine) and can be induced by pathways that sense demand for detoxification and for modulation of endobiotic signaling molecules. The functions of the UGT3 and UGT8 family enzymes have only been characterized relatively recently; these enzymes show different UDP-sugar preferences to that of UGT1 and UGT2 enzymes, and to date, their contributions to drug metabolism appear to be relatively minor. This review summarizes and provides critical analysis of the current state of research into all four families of UGT enzymes. Key areas discussed include the roles of UGTs in drug metabolism, cancer risk, and regulation of signaling, as well as the transcriptional and posttranscriptional control of UGT expression and function. The latter part of this review provides an in-depth analysis of the known and predicted functions of UGT3 and UGT8 enzymes, focused on their likely roles in modulation of levels of endogenous signaling pathways.

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Section: Ugt8 Outside Of the Nervous System: Kidney Testis Bone Marrow And Cancer Cellssupporting

confidence: 63%

Section: Ugt8 Outside Of the Nervous System: Kidney Testis Bone Marrow And Cancer Cellsmentioning

confidence: 53%

The UDP-Glycosyltransferase (UGT) Superfamily: New Members, New Functions, and Novel Paradigms

Meech

McKinnon

et al. 2019

Physiological Reviews

193

128

View full text Add to dashboard Cite

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“…Fluorescent labelling of sphingolipids was previously used to study their trafficking, uptake, and metabolism, where it was proven to be a powerful tool, specifically in the trafficking of ceramide to the Golgi- apparatus [41, 42]. Furthermore, emerging reports [24, 43, 44] indicated elevated levels of UGT8 in breast cancer and lung metastasis, and have suggested using UGT8 as a biomarker in the cancer prognosis. Nevertheless, no comprehensive molecular analysis of the signaling mechanism of this molecule is available.…”

Section: Discussionmentioning

confidence: 99%

“…This enzyme is localized to the nuclear envelope and the endoplasmic reticulum and has been reported to act as an anti-apoptotic molecule that affects tumorigenic and metastatic properties of breast cancer cells [22]. UGT8 is also linked to the development of lung metastases and is up-regulated in both ovarian and breast cancers [23–25]. Its anti-apoptotic function is achieved through disruption of the ceramide signalling pathway by converting ceramide into galactosylceramide.…”

Section: Introductionmentioning

confidence: 99%

Microbubble-based enhancement of radiation effect: Role of cell membrane ceramide metabolism

et al. 2017

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Ultrasound (US) stimulated microbubbles (MB) is a new treatment approach that sensitizes cancer cells to radiation (XRT). The molecular pathways in this response remain unelucidated, however, previous data has supported a role for cell membrane-metabolism related pathways including an up regulation of UDP glycosyltransferase 8 (UGT8), which catalyzes the transfer of galactose to ceramide, a lipid that is associated with the induction of apoptotic signalling. In this study, the role of UGT8 in responses of prostate tumours to ultrasound-stimulated microbubble radiation enhancement therapy is investigated. Experiments were carried out with cells in vitro and tumours in vivo in which UGT8 levels had been up regulated or down regulated. Genetically modified PC3 cells were treated with XRT, US+MB, or a combination of XRT+US+MB. An increase in the immunolabelling of ceramide was observed in cells where UGT8 was down-regulated as opposed to cells where UGT8 was either not regulated or was up-regulated. Clonogenic assays have revealed a decreased level of cellular survival with the down-regulation of UGT8. Xenograft tumours generated from stably transfected PC3 cells were also treated with US+MB, XRT or US+MB+XRT. Histology demonstrated more cellular damage in tumours with down-regulated UGT8 in comparison with control tumours. In contrast, tumours with up-regulated UGT8 had less damage than control tumours. Power Doppler imaging indicated a reduction in the vascular index with UGT8 down-regulation and photoacoustic imaging revealed a reduction in oxygen saturation. This was contrary to when UGT8 was up regulated. The down regulation of UGT8 led to the accumulation of ceramide resulting in more cell death signalling and therefore, a greater enhancement of radiation effect when vascular disruption takes place through the use of ultrasound-stimulated microbubbles.

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“…UGT8 was recently reported to be highly expressed in breast tumors with a malignant phenotype but not in nonmetastatic tumors (Dzięgiel et al, 2010). Several publications now posit UGT8 as a marker of cancer malignancy (Nowak et al, 2013;Owczarek et al, 2013): production of GalCer by UGT8 may alter cancer cell adhesion and also inhibit apoptosis (Beier and Gorogh, 2005;Owczarek et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

A Novel Function for UDP Glycosyltransferase 8: Galactosidation of Bile Acids

et al. 2014

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The human UDP glycosyltransferase (UGT) superfamily comprises four families of enzymes that catalyze the addition of sugar residues to small lipophilic chemicals. The UGT1 and UGT2 enzymes use UDP-glucuronic acid, and UGT3 enzymes use UDP-N-acetylglucosamine, UDP-glucose, and UDP-xylose to conjugate xenobiotics, including drugs and endobiotics such as metabolic byproducts, hormones, and signaling molecules. This metabolism renders the substrate more polar and more readily excreted from the body and/or functionally inactive. The fourth UGT family, called UGT8, contains only one member that, unlike other UGTs, is considered biosynthetic. UGT8 uses UDP galactose to galactosidate ceramide, a key step in the synthesis of brain sphingolipids. To date other substrates for this UGT have not been identified and there has been no suggestion that UGT8 is involved in metabolism of endo-or xenobiotics. We reexamined the functions of UGT8 and discovered that it efficiently galactosidates bile acids and drug-like bile acid analogs. UGT8 conjugates bile acids ∼60-fold more efficiently than ceramide based on in vitro assays with substrate preference deoxycholic acid . chenodeoxycholic acid . cholic acid . hyodeoxycholic acid . ursodeoxycholic acid. Activities of human and mouse UGT8 are qualitatively similar. UGT8 is expressed at significant levels in kidney and gastrointestinal tract (intestine, colon) where conjugation of bile acids is likely to be metabolically significant. We also investigate the structural determinants of UDP-galactose selectivity. Our novel findings suggest a new role for UGT8 as a modulator of bile acid homeostasis and signaling.

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Ceramide galactosyltransferase (UGT8) as a molecular marker of canine mammary tumor malignancy

Cited by 8 publications

References 18 publications

The UDP-Glycosyltransferase (UGT) Superfamily: New Members, New Functions, and Novel Paradigms

The UDP-Glycosyltransferase (UGT) Superfamily: New Members, New Functions, and Novel Paradigms

Microbubble-based enhancement of radiation effect: Role of cell membrane ceramide metabolism

A Novel Function for UDP Glycosyltransferase 8: Galactosidation of Bile Acids

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