TY - JOUR
T1 - Harly endothelium activation and polymorphonuclear cell invasion precede specific necrosis of human melanoma and sarcoma treated by intravascular high‐dose tumour necrosis factor alpha (rTNFα)
AU - Renard, N.
AU - Liénard, D.
AU - Lespagnard, L.
AU - Eggermont, A.
AU - Heimann, R.
AU - Lejeune, F.
PY - 1994/6/1
Y1 - 1994/6/1
N2 - Twenty‐seven patients treated with high‐dose rTNFα, IFNγ and melphalan by isolated limb perfusion were histologically documented. There were 20 cases of melanoma‐in‐transit metastases and 7 cases of high‐grade soft‐tissue sarcoma. Biopsies were taken before IFN7, after IFNγ, before TNFα and between 2 hr and 60 days after the TNFα perfusion. Immunohistochemistry was performed for adhesion molecules ICAM‐I, ELAM‐I (E selectin), VCAM‐I and PECAM. During the first hours after beginning perfusion, the endothelial cells of the tumour capillaries appeared swollen. Significant tumour necrosis was already observed 3 hours after the perfusion in melanoma cases. The overall predominant feature was coagulative necrosis associated or not with haemorrhagic necrosis. TNFα induced increased expression of ELAM‐I and VCAM‐I adhesion molecules on intratumoral endothelial cells. The activated tumour vessels were progressively destroyed. Significant intra‐vascular recruitment of polymorphonuclear cells (PMNs) was observed 3 hr after starting TNFα; it was followed by diapedesis and tumour colonization 3 days later. T lymphocytes and macrophages were detected during the first 7 days and B lymphocytes during the second week. Melanoma in transit metastases treated with alkylating agent alone did not show significant necrosis and did not express high levels of adhesion molecules (ELAM‐1, VCAM‐I) nor infiltration by PMN.
AB - Twenty‐seven patients treated with high‐dose rTNFα, IFNγ and melphalan by isolated limb perfusion were histologically documented. There were 20 cases of melanoma‐in‐transit metastases and 7 cases of high‐grade soft‐tissue sarcoma. Biopsies were taken before IFN7, after IFNγ, before TNFα and between 2 hr and 60 days after the TNFα perfusion. Immunohistochemistry was performed for adhesion molecules ICAM‐I, ELAM‐I (E selectin), VCAM‐I and PECAM. During the first hours after beginning perfusion, the endothelial cells of the tumour capillaries appeared swollen. Significant tumour necrosis was already observed 3 hours after the perfusion in melanoma cases. The overall predominant feature was coagulative necrosis associated or not with haemorrhagic necrosis. TNFα induced increased expression of ELAM‐I and VCAM‐I adhesion molecules on intratumoral endothelial cells. The activated tumour vessels were progressively destroyed. Significant intra‐vascular recruitment of polymorphonuclear cells (PMNs) was observed 3 hr after starting TNFα; it was followed by diapedesis and tumour colonization 3 days later. T lymphocytes and macrophages were detected during the first 7 days and B lymphocytes during the second week. Melanoma in transit metastases treated with alkylating agent alone did not show significant necrosis and did not express high levels of adhesion molecules (ELAM‐1, VCAM‐I) nor infiltration by PMN.
UR - http://www.scopus.com/inward/record.url?scp=0028232019&partnerID=8YFLogxK
U2 - 10.1002/ijc.2910570508
DO - 10.1002/ijc.2910570508
M3 - Article
C2 - 8194873
AN - SCOPUS:0028232019
SN - 0020-7136
VL - 57
SP - 656
EP - 663
JO - International Journal of Cancer
JF - International Journal of Cancer
IS - 5
ER -