Literature DB >> 11027431

Nitric oxide synthase inhibition results in synergistic anti-tumour activity with melphalan and tumour necrosis factor alpha-based isolated limb perfusions.

J H de Wilt1, E R Manusama, B van Etten, S T van Tiel, A S Jorna, A L Seynhaeve, T L ten Hagen, A M Eggermont.   

Abstract

Nitric oxide (NO) is an important molecule in regulating tumour blood flow and stimulating tumour angiogenesis. Inhibition of NO synthase by L-NAME might induce an anti-tumour effect by limiting nutrients and oxygen to reach tumour tissue or affecting vascular growth. The anti-tumour effect of L-NAME after systemic administration was studied in a renal subcapsular CC531 adenocarcinoma model in rats. Moreover, regional administration of L-NAME, in combination with TNF and melphalan, was studied in an isolated limb perfusion (ILP) model using BN175 soft-tissue sarcomas. Systemic treatment with L-NAME inhibited growth of adenocarcinoma significantly but was accompanied by impaired renal function. In ILP, reduced tumour growth was observed when L-NAME was used alone. In combination with TNF or melphalan, L-NAME increased response rates significantly compared to perfusions without L-NAME (0-64% and 0-63% respectively). An additional anti-tumour effect was demonstrated when L-NAME was added to the synergistic combination of melphalan and TNF (responses increased from 70 to 100%). Inhibition of NO synthase reduces tumour growth both after systemic and regional (ILP) treatment. A synergistic anti-tumour effect of L-NAME is observed in combination with melphalan and/or TNF using ILP. These results indicate a possible role of L-NAME for the treatment of solid tumours in a systemic or regional setting. Copyright 2000 Cancer Research Campaign.

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Year:  2000        PMID: 11027431      PMCID: PMC2363576          DOI: 10.1054/bjoc.2000.1447

Source DB:  PubMed          Journal:  Br J Cancer        ISSN: 0007-0920            Impact factor:   7.640


  42 in total

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8.  Prerequisites for effective isolated limb perfusion using tumour necrosis factor alpha and melphalan in rats.

Authors:  J H de Wilt; E R Manusama; S T van Tiel; M G van Ijken; T L ten Hagen; A M Eggermont
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9.  TNF-alpha augments intratumoural concentrations of doxorubicin in TNF-alpha-based isolated limb perfusion in rat sarcoma models and enhances anti-tumour effects.

Authors:  A H van der Veen; J H de Wilt; A M Eggermont; S T van Tiel; A L Seynhaeve; T L ten Hagen
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10.  Tumour necrosis factor alpha increases melphalan concentration in tumour tissue after isolated limb perfusion.

Authors:  J H de Wilt; T L ten Hagen; G de Boeck; S T van Tiel; E A de Bruijn; A M Eggermont
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5.  Isolated limb perfusion with actinomycin D and TNF-alpha results in improved tumour response in soft-tissue sarcoma-bearing rats but is accompanied by severe local toxicity.

Authors:  A L B Seynhaeve; J H W de Wilt; S T van Tiel; A M M Eggermont; T L M ten Hagen
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