Publication

Monitoring tumor response during photodynamic therapy using near-infrared photon-migration spectroscopy

Journal Paper/Review - Jun 2, 2001

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Citation
Hornung R, Berns W, Tadir Y, Tromberg B, Phamt T. Monitoring tumor response during photodynamic therapy using near-infrared photon-migration spectroscopy. Photochemistry and Photobiology 2001; 73:669-677.
Type
Journal Paper/Review (English)
Journal
Photochemistry and Photobiology 2001; 73
Publication Date
Jun 2, 2001
Pages
669-677
Brief description/objective

Benzoporphyrin-derivative (BPD)–monoacid-ring A photodynamic therapy (PDT) was performed on subcutaneous tumor implants in a rat ovarian cancer model. In order to assess PDT efficacy the tumor and normal tissue optical properties were measured noninvasively prior to and during PDT using frequency-domain photon migration (FDPM). FDPM data were used to quantify tissue absorption and reduced scattering properties (given by the parameters μa and μ′s, respectively) at four near-infrared (NIR) wavelengths (674, 811, 849 and 956 nm). Tissue physiologic properties, including the in vivo concentration of BPD, deoxy-hemoglobin (Hb), oxy-hemoglobin (HbO2), total hemoglobin (TotHb), water (H2O) and percent tissue hemoglobin oxygen saturation (%StO2), were calculated from optical property data. PDT efficacy was also determined from morphometric analysis of tumor necrosis in histologic specimens. All the measured tumor properties changed significantly during PDT. [Hb] increased by 9%, while [HbO2], [TotHb] and %StO2 decreased by 18, 7 and 12%, respectively. Using histologic data we show that long-term PDT efficacy is highly correlated to mean BPD concentration in tumor and PDT-induced acute changes in [HbO2], [TotHb] and %StO2 (correlation coefficients of 0.829, 0.817 and 0.953, respectively). Overall, our results indicate that NIR FDPM spectroscopy is able to quantify noninvasively and dynamically the PDT-induced physiological effects in vivo that are highly correlated with therapeutic efficacy.