Vascular function and the probability of skin necrosis after photodynamic therapy: an experimental study.
Affiliation
Paterson Institute for Cancer Research, Christie Hospital and Holt Radium Institute, Manchester, UK.Issue Date
1988-05
Metadata
Show full item recordAbstract
The clearance of an intradermally-injected solution of 133Xenon in 0.9% saline has been used to study the impairment and recovery of blood flow in mouse tail for 5 days following photodynamic therapy (PDT) with 2mg TPPS i.v. per mouse and a range of doses of white light. Impairment of blood flow was observed within 10 min of light exposure. Blood flow increased between day 1 and day 5 at light doses less than 151J cm-2 and had returned to control levels by day 5 at light doses less than 129J cm-2. In mice treated with a light dose that caused a 50% incidence of necrosis, there was no significant difference in the initial xenon clearance half-time (measured at 10 min and 1 day after PDT) between those mice which developed tail necrosis and those which healed. However, the latter showed significantly greater improvement in vascular function on days 2, 3 and 4. This suggests that the timing and extent of recovery of blood flow determined the risk of necrosis in individual mice.Citation
Vascular function and the probability of skin necrosis after photodynamic therapy: an experimental study. 1988, 57 (5):451-4 Br J CancerJournal
British Journal of CancerPubMed ID
3395550Type
ArticleLanguage
enISSN
0007-0920Collections
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