Systematic analysis of the human tumor cell binding to human vs. murine E- and P-selectin under static vs. dynamic conditions

Starzonek, Sarah; Maar, Hanna; Labitzky, Vera; Wicklein, Daniel; Rossdam, Charlotte; Buettner, Falk F. R.; Wolters‐Eisfeld, Gerrit; Guengoer, Cenap; Wagener, Christoph; Schumacher, Udo; Lange, Tobias

doi:10.1093/glycob/cwaa019

Cited by 15 publications

(36 citation statements)

References 39 publications

(50 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Due to the ability to act as selectin ligands, both sLea and the type 2 chain isomer sialyl-Lewis x (Siaα2,3Galβ1,4[Fucα1,3]GlcNAc, in which the galactose residue is linked to N-acetylglucosamine through a β1,4 linkage), have been extensively investigated in recent years (reviewed in [ 35 , 36 ]). Because of their capacity to enhance the malignant potential of cancer cells, as proven in model systems [ 36 , 37 ]), it is important to assess the actual expression of such structures by native cancers [ 38 , 39 ] compared to the normal counterpart. The ability to synthesize the various epitopes depends on the expression of specific glycosyltransferase enzymatic activities.…”

Section: Biosynthesis Of Type 1 Chain Lewis Antigens In Gastrointementioning

confidence: 99%

Complementary Use of Carbohydrate Antigens Lewis a, Lewis b, and Sialyl-Lewis a (CA19.9 Epitope) in Gastrointestinal Cancers: Biological Rationale towards a Personalized Clinical Application

Indellicato

Zulueta

Caretti

et al. 2020

Cancers

View full text Add to dashboard Cite

Carbohydrate antigen 19.9 (CA19.9) is used as a tumor marker for clinical and research purposes assuming that it is abundantly produced by gastrointestinal cancer cells due to a cancer-associated aberrant glycosylation favoring its synthesis. Recent data has instead suggested a different picture, where immunodetection on tissue sections matches biochemical and molecular data. In addition to CA19.9, structurally related carbohydrate antigens Lewis a and Lewis b are, in fact, undetectable in colon cancer, due to the down-regulation of a galactosyltransferase necessary for their synthesis. In the pancreas, no differential expression of CA19.9 or cognate glycosyltransferases occurs in cancer. Ductal cells only express such Lewis antigens in a pattern affected by the relative levels of each glycosyltransferase, which are genetically and epigenetically determined. The elevation of circulating antigens seems to depend on the obstruction of neoplastic ducts and loss of polarity occurring in malignant ductal cells. Circulating Lewis a and Lewis b are indeed promising candidates for monitoring pancreatic cancer patients that are negative for CA19.9, but not for improving the low diagnostic performance of such an antigen. Insufficient biological data are available for gastric and bile duct cancer. Studying each patient in a personalized manner determining all Lewis antigens in the surgical specimens and in the blood, together with the status of the tissue-specific glycosylation machinery, promises fruitful advances in translational research and clinical practice.

show abstract

Section: Biosynthesis Of Type 1 Chain Lewis Antigens In Gastrointementioning

confidence: 99%

Complementary Use of Carbohydrate Antigens Lewis a, Lewis b, and Sialyl-Lewis a (CA19.9 Epitope) in Gastrointestinal Cancers: Biological Rationale towards a Personalized Clinical Application

Indellicato

Zulueta

Caretti

et al. 2020

Cancers

View full text Add to dashboard Cite

show abstract

“…Furthermore, not only different P-selectin levels on activated human vs. murine platelets, but also different ligands at the tumor cell surface used for binding human vs. murine Pselectin have to be considered: as reported quite recently, there is considerably more murine than human P-selectin binding to human tumor cells particularly when tumor cells express both canonical selectin ligands, i.e., the glycan epitopes sialyl-Lewis A and X (sLeA+/X+); there was much less difference seen with sLeA-/ sLeX+ or sLeA-/ sLeX-cells suggesting that the sLeA epitope (capping a variety of different carbohydrate structures) might specifically support murine P-selectin binding (109). All tested tumor cell lines stemming from a range of entities shared the ability to bind human and murine P-selectin, again underlining the crucial importance of P-selectin in the context of cancer.…”

Section: The Role Of P-selectin For the Platelet-tumor Cell Interactionmentioning

confidence: 99%

“…All tested tumor cell lines stemming from a range of entities shared the ability to bind human and murine P-selectin, again underlining the crucial importance of P-selectin in the context of cancer. Interestingly, several tumor cell treatments aiming at disrupting tumor cell/ P-selectin interaction impaired human vs. murine P-selectin binding quite differently suggesting that different ligands are functional for both species (109). Another dimension of complexity results from the differential binding and adhesion behavior of human tumor cells to murine vs. human P-selectin under static and dynamic experimental conditions, respectively: while all tested human tumor cells bound human and murine P-selectin under static conditions, only sLeA+/X+ and sLeX+ cells (but not sLeA-/sLeX-cells) were able to adhere dynamically on murine P-selectin.…”

Section: The Role Of P-selectin For the Platelet-tumor Cell Interactionmentioning

confidence: 99%

“…Interestingly, several tumor cell treatments aiming at disrupting tumor cell/ P-selectin interaction impaired human vs . murine P-selectin binding quite differently suggesting that different ligands are functional for both species ( 109 ). Another dimension of complexity results from the differential binding and adhesion behavior of human tumor cells to murine vs .…”

Section: The Role Of P-selectin For the Platelet-tumor Cell Interactimentioning

confidence: 99%

“…human P-selectin under static and dynamic experimental conditions, respectively: while all tested human tumor cells bound human and murine P-selectin under static conditions, only sLeA+/X+ and sLeX+ cells (but not sLeA-/sLeX- cells) were able to adhere dynamically on murine P-selectin. Among them, only those co-expressing PSGL-1 were able to adhere dynamically on human P-selectin ( 109 ). These observations imply that the ability of human tumor cells to directly interact with platelets inside the bloodstream (dynamic conditions) or outside the bloodstream (static conditions) might be remarkably different in mice and men.…”

Section: The Role Of P-selectin For the Platelet-tumor Cell Interactimentioning

confidence: 99%

See 2 more Smart Citations

The Role of Platelet Cell Surface P-Selectin for the Direct Platelet-Tumor Cell Contact During Metastasis Formation in Human Tumors

2021

Self Cite

View full text Add to dashboard Cite

Mammalian platelets, devoid of nuclei, are the smallest cells in the blood stream. They are essential for hemostasis, but also transmit cell signals that are necessary for regenerative and generative processes such as inflammation, immunity and tissue repair. In particular, in malignancies they are also associated with cell proliferation, angiogenesis, and epithelial-mesenchymal transition. Platelets promote metastasis and resistance to anti-tumor treatment. However, fundamental principles of the interaction between them and target cells within tumors are complex and still quite obscure. When injected into animals or circulating in the blood of cancer patients, cancer cells ligate platelets in a timely manner closely related to platelet activation either by direct contact or by cell-derived substances or microvesicles. In this context, a large number of different surface molecules and transduction mechanisms have been identified, although the results are sometimes species-specific and not always valid to humans. In this mini-review, we briefly summarize the current knowledge on the role of the direct and indirect platelet-tumor interaction for single steps of the metastatic cascade and specifically focus on the functional role of P-selectin.

show abstract

Glycosylation as a regulator of site-specific metastasis

Bindeman

Fingleton

2021

Cancer Metastasis Rev

View full text Add to dashboard Cite

Systematic analysis of the human tumor cell binding to human vs. murine E- and P-selectin under static vs. dynamic conditions

Cited by 15 publications

References 39 publications

Complementary Use of Carbohydrate Antigens Lewis a, Lewis b, and Sialyl-Lewis a (CA19.9 Epitope) in Gastrointestinal Cancers: Biological Rationale towards a Personalized Clinical Application

Complementary Use of Carbohydrate Antigens Lewis a, Lewis b, and Sialyl-Lewis a (CA19.9 Epitope) in Gastrointestinal Cancers: Biological Rationale towards a Personalized Clinical Application

The Role of Platelet Cell Surface P-Selectin for the Direct Platelet-Tumor Cell Contact During Metastasis Formation in Human Tumors

Glycosylation as a regulator of site-specific metastasis

Contact Info

Product

Resources

About