Literature DB >> 7536022

Transient perfusion in human melanoma xenografts.

I Tufto1, E K Rofstad.   

Abstract

Studies of transplantable rodent tumours have suggested that malignant tissue might experience transient perfusion at the microvascular level. The purpose of the work reported here was to investigate whether transient perfusion can be demonstrated in xenografted human tumours. Tumours of four melanoma lines (A-07, D-12, R-18, U-25), grown orthotopically in Balb/c nu/nu mice, were included in the study. Transient perfusion was studied by using the double-fluorescent staining technique. Hoechst 33342 and DiOC7(3) were either administered simultaneously or Hoechst 33342 was administered 20 min before DiOC7(3). Detection of transient perfusion by this method requires that vessels are non-functional for at least 5 min owing to the distribution half-lives of the dyes in the blood. Usable combinations of dye concentrations were found by varying the concentrations of Hoechst 33342 and DiOC7(3) systematically. The level of perfusion mismatch following simultaneous administration of the dyes ranged from approximately 1.5% for U-25 tumours to approximately 3.0% for R-18 tumours at these combinations. Moreover, the fraction of vessels stained only with Hoechst 33342 and the fraction of vessels stained only with DiOC7(3) were not significantly different whether the dyes were administered simultaneously or sequentially. Transient perfusion could not be demonstrated in any of the tumour lines. Thus, the fraction of vessels stained only with Hoechst 33342 and the fraction of vessels stained only with DiOC7(3) were not significantly higher after sequential than after simultaneous administration of the dyes. Moreover, the vessels stained only with Hoechst 33342 and the vessels stained only with DiOC7(3) were randomly distributed within the tumours whether the dyes were administered simultaneously or sequentially. Consequently, acute hypoxia caused by transient perfusion is probably a less pronounced phenomenon in malignant tissue than previous studies of rodent tumours have suggested.

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Year:  1995        PMID: 7536022      PMCID: PMC2033749          DOI: 10.1038/bjc.1995.153

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


  31 in total

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Journal:  Int J Radiat Oncol Biol Phys       Date:  1986-08       Impact factor: 7.038

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Journal:  Br J Cancer       Date:  1988-09       Impact factor: 7.640

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Journal:  Br J Cancer       Date:  1955-12       Impact factor: 7.640

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  4 in total

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Authors:  C Bayer; P Vaupel
Journal:  Strahlenther Onkol       Date:  2012-03-29       Impact factor: 3.621

2.  Quantitative assessment of hypoxia subtypes in microcirculatory supply units of malignant tumors using (immuno-)fluorescence techniques.

Authors:  Constantin-Alin Maftei; Christine Bayer; Kuangyu Shi; Sabrina T Astner; Peter Vaupel
Journal:  Strahlenther Onkol       Date:  2011-03-24       Impact factor: 3.621

3.  Suppression of HIF-1α expression and radiation resistance in acute hypoxic conditions.

Authors:  Takahiro Oike; Yoshiyuki Suzuki; Wael Al-Jahdari; Abdulelah Mobaraki; Jun-Ichi Saitoh; Kohta Torikai; Katsuyuki Shirai; Takashi Nakano
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4.  Growth rates or radiobiological hypoxia are not correlated with local metabolite content in human melanoma xenografts with similar vascular network.

Authors:  M Kroeger; S Walenta; E K Rofstad; W Mueller-Klieser
Journal:  Br J Cancer       Date:  1995-10       Impact factor: 7.640

  4 in total

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