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Jan Joseph

Researcher at Witten/Herdecke University

Publications -  8
Citations -  1226

Jan Joseph is an academic researcher from Witten/Herdecke University. The author has contributed to research in topics: Cell migration & Receptor. The author has an hindex of 8, co-authored 8 publications receiving 1159 citations.

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Tumour-cell migration, invasion, and metastasis: navigation by neurotransmitters.

TL;DR: This work has shown that many types of neurotransmitter receptors are expressed on tumour cells, supporting the theory that psychosocial factors are involved in the progression of cancer, and could open up new avenues for chemoprevention of tumour-cell migration and metastatic development.
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Effects of neurotransmitters on the chemokinesis and chemotaxis of MDA-MB-468 human breast carcinoma cells.

TL;DR: Evidence is provided for a strong regulatory involvement of neurotransmitters in the regulation of breast cancer cell migration, which might provide the basis for the use of the pharmacological agonists and antagonists for the chemopreventive inhibition of metastasis development.

Iconography : Tumour-cell migration, invasion, and metastasis: navigation by neurotransmitters

TL;DR: The most prominent regulatory factors are ligands to serpentine receptors-eg, chemokines and neurotransmitters as mentioned in this paper, which are involved in the migration of cancer cells into surrounding tissues, resulting in development of distant metastases.
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Anandamide is an endogenous inhibitor for the migration of tumor cells and T lymphocytes

TL;DR: The inhibitory effect of the endogenous substance anandamide on both tumor cell and lymphocyte migration is reported, suggesting specific inhibition of tumor cell migration via CB1-R engagement might be a selective tool to prevent metastasis formation without depreciatory effects on the immune system of cancer patients.
Journal Article

The Neurotransmitter γ-Aminobutyric Acid Is an Inhibitory Regulator for the Migration of SW 480 Colon Carcinoma Cells

TL;DR: GABA reduced the norepinephrine-induced migratory activity of cells within a three-dimensional collagen matrix to spontaneous migration levels, opening new possibilities for pharmacological agonists in cancer therapy.