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Margot Zöller

Researcher at Heidelberg University

Publications -  251
Citations -  16514

Margot Zöller is an academic researcher from Heidelberg University. The author has contributed to research in topics: CD44 & Antigen. The author has an hindex of 56, co-authored 250 publications receiving 15289 citations. Previous affiliations of Margot Zöller include Merck & Co. & German Cancer Research Center.

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A new variant of glycoprotein cd44 confers metastatic potential to rat carcinoma cells

TL;DR: Using a monoclonal antibody raised against a surface glycoprotein of the metastasizing rat pancreatic carcinoma cell line BSp73ASML, cDNA clones have been isolated that encode glycoproteins with partial homology to CD44, a presumed adhesion molecule.
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CD44: can a cancer-initiating cell profit from an abundantly expressed molecule?

TL;DR: Can an abundantly expressed molecule be a reliable marker for the cancer-initiating cells (CICs) and is CD44 expression advantageous as it fulfils some of the special properties that are displayed by CICs, such as self-renewal, niche preparation, epithelial–mesenchymal transition and resistance to apoptosis?
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Tetraspanins: push and pull in suppressing and promoting metastasis

TL;DR: It is reasonable to assume that differences in the membrane and vesicular web components that associate with individual tetraspanins account for their differing abilities to promote and suppress metastasis.
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Cell surface tetraspanin Tspan8 contributes to molecular pathways of exosome-induced endothelial cell activation.

TL;DR: EC uptake of Tspan8-CD49d complex-containing exosomes was accompanied by enhanced EC proliferation, migration, sprouting, and maturation of EC progenitors, which could provide new options for therapeutic interference with tumor-induced angiogenesis.
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Toward tailored exosomes: The exosomal tetraspanin web contributes to target cell selection

TL;DR: This is the first report on the exosomal tetraspanin web contributing to target cell selection such that predictions can be made on potential targets, which will facilitate tailoring exosomes for drug delivery.