✦ LIBER ✦

Preclinical in vivo evaluation of Npe6-mediated photodynamic therapy on normal vasculature

✍ Scribed by Wesley J. Moy; Shreyas J. Patel; Ben S. Lertsakdadet; Rajan P. Arora; Katherine M. Nielsen; Kristen M. Kelly; Bernard Choi

Book ID: 102465889
Publisher: John Wiley and Sons
Year: 2012
Tongue: English
Weight: 143 KB
Volume: 44
Category: Article
ISSN: 0196-8092
DOI: 10.1002/lsm.21155

No coin nor oath required. For personal study only.

✦ Synopsis

Abstract

Background and Objective

Current treatments of port‐wine stain birthmarks typically involve use of a pulsed dye laser (PDL) combined with cooling of the skin. Currently, PDL therapy protocols result in varied success, as some patients experience complete blanching, while others do not. Over the past decade, we have studied the use of photodynamic therapy (PDT) as either a replacement or adjuvant treatment option to photocoagulate both small and large vasculature. The objective of the current study was to evaluate a PDT protocol that involves use of an alternate intravascular photosensitizer mono‐L‐aspartylchlorin‐e6 (NPe6) activated by an array of low‐cost light emitting diodes.

Study Design/Materials and Methods

To monitor the microvasculature, a dorsal window chamber model was installed on 22 adult male mice. The light source consisted of a custom‐built LED array that emitted 10 W at a center wavelength of 664 nm (FWHM = 20 nm). The light source was positioned at a fixed distance from the window chamber to achieve a fixed irradiance of 127 mW/cm^2^. A retroorbital injection of NPe6 (5 mg/kg) was performed to deliver the drug into the bloodstream. Laser irradiation was initiated immediately after injection. To monitor blood‐flow dynamics in response to PDT, we used laser speckle imaging. We employed a dose–response experimental design to evaluate the efficacy of NPe6‐mediated PDT.

Results

We observed three general hemodynamic responses to PDT: (1) At low radiant exposures, we did not observe any persistent vascular shutdown; (2) at intermediate radiant exposures, we observed an acute decrease in blood flow followed by gradual restoration of blood flow over the 7‐day monitoring period; and (3) at high radiant exposures, we observed acute vascular shutdown that persisted during the entire 7‐day monitoring period. Dose–response analysis enabled identification of 85 J/cm^2^ as a characteristic radiant exposure required to achieve persistent vascular shutdown at Day 7 following PDT.

Conclusion

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