Foscan-mediated photodynamic therapy and operation for malignant pleural mesothelioma

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Foscan-mediated photodynamic therapy and operation for malignant pleural mesothelioma

Hugo Schouwink, MD, PhD, Paul Baas, MD, PhD

Department of Thoracic Oncology, The Netherlands Cancer Institute, Plesmanlaan 121, 1066 CX, Amsterdam, The Netherlands

e-mail: j.schouwink{at}ziekenhuis-mst.nl

To the Editor:

With great interest we read the article by Friedberg and associates[1] about operation and m-THPC (meta-tetrahydroxyphenylchlorin)–mediatedphotodynamic therapy (PDT) in patients with malignant pleuralmesothelioma. This phase I study is an important contributionto understanding the potential role of PDT in this disease.

In 2001, we [2] reported the results of a phase I/II study ofsurgical intervention and m-THPC–mediated PDT in patientswith malignant pleural mesothelioma. When we compared thesetwo studies, we found many likenesses. The total number of patientstreated was similar, as was the number of patients treated atthe maximum tolerated dose. Median survival was 12.4 monthsin the study by Friedberg and colleagues versus 10 months inour study, but the difference is probably not significant.

An important difference between the studies was the intervalbetween injection of the photosensitizer and illumination. Theinterval was 6 days in the Friedberg study versus 4 days inours. The light and sensitizer doses were comparable. All ourpatients had a pleuropneumonectomy, which facilitated illuminationof the chest cavity. Illumination is much more complicated whenthe lung remains in situ. Two patients died after developmentof a pulmonary capillary leak syndrome after PDT in the studyof Friedberg and co-workers. This may have been related to thelarge illuminated surface of the lung. On the other hand, themorbidity and the mortality associated with pleuropneumonectomyare also considerable.

One of the problems of this combined modality approach is separatingsurgical and PDT–related toxicity. A significant reductionin toxicity is most likely achieved by modifications to thePDT part of the combined treatment. For this purpose, Friedbergand colleagues prolonged the drug-light interval to 6 days.Other options to reduce the undesired PDT effect on normal tissuesinclude the reduction in drug and light doses or the use ofless potent photosensitizers.

When the combination of limited resection and reduced PDT efficacyis explored, two issues deserve special attention during preoperativeanalysis. First, the total tumor volume should be taken intoaccount [3]. Patients with massive tumors are at great riskfor postoperative side effects. Assessment of viable tumor canbe performed with three-dimensional reconstruction of computedtomographic scans or magnetic resonance images in combinationwith position emission tomographic scanning [4]. Second, iflung tissue remains during PDT illumination, light distributioncannot be monitored optimally.

It seems unlikely that proper light distribution in this situationcan be achieved with only four light detectors. The most obviousway to improve light distribution is to incorporate more thanfour light detectors in the chest cavity. However, illuminationof the diaphragmatic gutter will remain problematic. In a systemwith integral illumination using one light source, as was donein both studies, the diaphragmatic sinus in many patients isshielded from light. In these patients, additional illuminationis required to achieve the PDT effect in the narrow space betweenthe diaphragm and the chest wall. In our opinion, improvementin PDT in this region can be achieved only with advanced techniquessuch as the one described by van Veen and co-authors [5].

Results of the combination of operation and m-THPC–mediatedPDT have not been very successful to date. Better treatmentoutcomes from future treatment protocols can be expected fromstricter patient selection and technical improvements in lightdosimetry. We believe that the results of the Friedberg studyindicate that the concept of limited resection in combinationwith relatively mild PDT deserves further investigation.

References

Friedberg J.S., Mick R., Stevenson J., et al. A phase I study of Foscan-mediated photodynamic therapy and surgery in patients with mesothelioma. Ann Thorac Surg 2003;75:952-959.[Abstract/Free Full Text]
Schouwink H., Rutgers E.T., van der Sijp J., et al. Intraoperative photodynamic therapy after pleuropneumonectomy in patients with malignant pleural mesothelioma: dose finding and toxicity results. Chest 2001;120:1167-1174.[Abstract/Free Full Text]
Pass H.W., Temeck B.K., Kranda K., Steinberg S.M., Pass H.I. A phase II trial investigating primary immunochemotherapy for malignant pleural mesothelioma and the feasibility of adjuvant immunochemotherapy after maximal cytoreduction. Ann Surg Oncol 1995;2:214-220.[Abstract]
Benard F., Sterman D., Smith R.J., Kaiser L.R., Albelda S.M., Alavi A. Metabolic imaging of malignant pleural mesothelioma with fluorodeoxyglucose positron emission tomography. Chest 1998;114:713-722.[Abstract/Free Full Text]
Van Veen P., Schouwink J.H., Star W.M., et al. Wedge-shaped applicator for additional light delivery and dosimetry in the diaphragmal sinus during photodynamic therapy for malignant pleural mesothelioma. Phys Med Biol 2001;46:1873-1883.[Medline]

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