Characterization of the specific response to serotonin of mouse tumour-feeding arterioles

Characterization of the specific response to serotonin of mouse tumour-feeding arterioles

Purpose: To investigate the role of tumour versus non-tumour factors in the specific response to serotonin (5-HT) of tumour-feeding arterioles (TFA). Materials and methods: Using mouse models of intra-vital microscopy, the response to topical administration of 5-HT was studied in arterioles feeding...

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Published in:International journal of radiation biology Vol. 74; no. 3; pp. 379 - 386
Main Authors: LAEMMEL, E, STÜCKER, O, DARMON, P.-L, VICAUT, E
Format: Journal Article
Language:English
Published: London Informa UK Ltd 1998
Taylor & Francis
Subjects:
Animals
Arterioles - drug effects
Arterioles - pathology
Axillary Artery - drug effects
Biological and medical sciences
Colorectal Neoplasms - blood supply
General aspects (metabolism, cell proliferation, established cell line...)
Humans
Medical sciences
Mice
Mice, Nude
Muscle, Skeletal - blood supply
Neoplasm Transplantation
Serotonin - administration & dosage
Serotonin - pharmacology
Skin - blood supply
Skin Neoplasms - blood supply
Space life sciences
Tumor cell
Tumors
Characterization
Vertebrata
Mammalia
Mouse
Serotonin
Arteriole
Animal
Rodentia
Established cell line
Tumor
Vascularization
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Summary:Purpose: To investigate the role of tumour versus non-tumour factors in the specific response to serotonin (5-HT) of tumour-feeding arterioles (TFA). Materials and methods: Using mouse models of intra-vital microscopy, the response to topical administration of 5-HT was studied in arterioles feeding tumours: fibrosarcoma (Meth A), murine mammary adenocarcinoma (EMT6) and human colo-rectal carcinoma (HRT18) intra-cutaneously implanted. Results: For all types of tumour, 5-HT induced a far more pronounced constriction of TFA than of control arterioles. The presence of a tumour implanted in the connective tissue between the skin and the cremaster muscle also affected the reactivity of muscle arterioles. Conversely, the response to serotonin by neovessels grown after implantation of an exogenous element under the skin did not differ from that of control arterioles. Conclusions: Changes in reactivity to serotonin were not dependent on the type of tumour implanted in the skin and were not present for a non-tumour implant. The presence of the tumour can alter the reactivity of vessels from tissue in contact with the tumour even if these vessels did not feed the tumour. This phenomenon is local and was not found in the vessels at a distance from the tumour.
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ISSN:0955-3002
1362-3095
DOI:10.1080/095530098141519