O activate the PS using ionizing radiation such as X-rays. Because X-rays are used for radiation therapy, each of these activation routes could be combined with radiotherapy to enhance the overall efficiency of the tumor treatment. Method 1 involves direct ONO-4059 structure excitation of the PS using ionizing radiation such as X-rays. In this case, the PSs are called radiosensitizers. Method 2 involves a local generation of light using the broad spectrum Cerenkov emission process, when a charged particle travels faster than light in a given matter and emits Cerenkov radiation. This emission presents a strong overlap with the absorption spectra of many PS and can subsequently be used to excite them. Method 3 shows the use of nanoscintillators that act as nanotransducers to locally convert ionizing radiation into visible light to excite PSs. The transfer from the nanoscintillator to the PS can either be radiative or non-radiative (FRET), and leads to activation of the PS. Abbreviations: NIR: Near Infrared, FL: Fluorescence, PH: Phosphorescence, ISC: Inter-System Crossing, MS: Metastable State, NRD: Non Radiative Decay, NER: Non-Elastic Relaxation and T: Thermalisation.http://www.thno.orgTheranostics 2016, Vol. 6, IssueTable 1: Photosensitizers designed and synthesized for TP-PDT. For each compound, the excitation wavelength (in nanometers), the TP absorption cross section (in GM; 1 GM = 10-50 cm4s.Photon-1) and the singlet oxygen quantum yield are indicated.Compound Excitation wavelength (nm) 802 TP absorption cross section (GM) 139 0.36 / 7600 8200 9100 1750 2280 17000 17400 6000 5.4.109 1556 251 0.46 / 0.84 0.54 0.78 0.23 0.60 0.33 0.51 1.10-2 0.49 0.80 RefSince TP excitation requires high incident laser intensity, the GNRs may undergo an irreversible deformation that leads to a loss of their emission properties. To prevent this type of photo-damage, Chen et al. synthesized mesoporous silica-encased GNRs that incorporate a PS for TP activated PDT and showed efficient generation of 1O2 and cell killing [88]. In addition to GNRs, QDs are potential candidates for TP mediated PS activation. In addition to exhibiting PS properties themselves [89, 90], QDs have demonstrated efficiency in acting as an energy transducer to activate PS bound to their surface via FRET [91]. These semi-conducting NPs are also characterized by a high TP absorption cross-section, making them uniquely suited for deep-tissue PDT. Because heavy metal containing QDs are quite toxic to cells, carbon QDs (CQD) appear as an attractive alternative. Fowley et al. reported the synthesis of high TP absorption cross-section CQDs combined with the PS PpIX. Under TP excitation, CQD absorb and transfer energy via FRET to the conjugated PS that then generates cytotoxic species. HeLa cells were exposed to different concentrations of CQD/PpIX conjugates and a viability reduction was demonstrated. In addition, the in vivo efficiency of this compound was shown in that it strongly reduced the size of fibrosarcoma tumors induced in mice [92]. Besides allowing for PDT activation at increased depth, TP-PDT also confines the excitation to the laser focal point. Though localized illumination of TP-PDT could be useful for purchase MS023 certain applications, it can be a major limitation and unrealistic from a practical viewpoint for treating large and disseminated tumors. Broad therapeutic strategies, such as single photon PDT, could be used to treat larger tumor regions while TP-PDT could be reserved for subsequent precise.O activate the PS using ionizing radiation such as X-rays. Because X-rays are used for radiation therapy, each of these activation routes could be combined with radiotherapy to enhance the overall efficiency of the tumor treatment. Method 1 involves direct excitation of the PS using ionizing radiation such as X-rays. In this case, the PSs are called radiosensitizers. Method 2 involves a local generation of light using the broad spectrum Cerenkov emission process, when a charged particle travels faster than light in a given matter and emits Cerenkov radiation. This emission presents a strong overlap with the absorption spectra of many PS and can subsequently be used to excite them. Method 3 shows the use of nanoscintillators that act as nanotransducers to locally convert ionizing radiation into visible light to excite PSs. The transfer from the nanoscintillator to the PS can either be radiative or non-radiative (FRET), and leads to activation of the PS. Abbreviations: NIR: Near Infrared, FL: Fluorescence, PH: Phosphorescence, ISC: Inter-System Crossing, MS: Metastable State, NRD: Non Radiative Decay, NER: Non-Elastic Relaxation and T: Thermalisation.http://www.thno.orgTheranostics 2016, Vol. 6, IssueTable 1: Photosensitizers designed and synthesized for TP-PDT. For each compound, the excitation wavelength (in nanometers), the TP absorption cross section (in GM; 1 GM = 10-50 cm4s.Photon-1) and the singlet oxygen quantum yield are indicated.Compound Excitation wavelength (nm) 802 TP absorption cross section (GM) 139 0.36 / 7600 8200 9100 1750 2280 17000 17400 6000 5.4.109 1556 251 0.46 / 0.84 0.54 0.78 0.23 0.60 0.33 0.51 1.10-2 0.49 0.80 RefSince TP excitation requires high incident laser intensity, the GNRs may undergo an irreversible deformation that leads to a loss of their emission properties. To prevent this type of photo-damage, Chen et al. synthesized mesoporous silica-encased GNRs that incorporate a PS for TP activated PDT and showed efficient generation of 1O2 and cell killing [88]. In addition to GNRs, QDs are potential candidates for TP mediated PS activation. In addition to exhibiting PS properties themselves [89, 90], QDs have demonstrated efficiency in acting as an energy transducer to activate PS bound to their surface via FRET [91]. These semi-conducting NPs are also characterized by a high TP absorption cross-section, making them uniquely suited for deep-tissue PDT. Because heavy metal containing QDs are quite toxic to cells, carbon QDs (CQD) appear as an attractive alternative. Fowley et al. reported the synthesis of high TP absorption cross-section CQDs combined with the PS PpIX. Under TP excitation, CQD absorb and transfer energy via FRET to the conjugated PS that then generates cytotoxic species. HeLa cells were exposed to different concentrations of CQD/PpIX conjugates and a viability reduction was demonstrated. In addition, the in vivo efficiency of this compound was shown in that it strongly reduced the size of fibrosarcoma tumors induced in mice [92]. Besides allowing for PDT activation at increased depth, TP-PDT also confines the excitation to the laser focal point. Though localized illumination of TP-PDT could be useful for certain applications, it can be a major limitation and unrealistic from a practical viewpoint for treating large and disseminated tumors. Broad therapeutic strategies, such as single photon PDT, could be used to treat larger tumor regions while TP-PDT could be reserved for subsequent precise.
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