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基于光漂白的方法实现 5-氨基酮戊酸光动力疗法间质内个体化照射时间。

Photobleaching-based method to individualize irradiation time during interstitial 5-aminolevulinic acid photodynamic therapy.

机构信息

Laser-Forschungslabor, LIFE Center, University Hospital of Munich, Marchioninistraße 23, 81377 Munich, Germany.

出版信息

Photodiagnosis Photodyn Ther. 2011 Sep;8(3):275-81. doi: 10.1016/j.pdpdt.2011.03.338. Epub 2011 Apr 2.

Abstract

Interstitial photodynamic therapy (iPDT) is being investigated for the treatment of high-grade human brain malignancies. In recent clinical studies, fluorescence monitoring during iPDT of glioblastoma multiforme has revealed patient-specific accumulation of photosensitizer (aminolevulinic acid (ALA) induced protoporphyrin IX, PpIX) and its photobleaching kinetics. As photosensitizer degradation, also referred to as photobleaching, and tissue damage are caused by the same underlying processes, the photobleaching kinetics might provide a tool for real-time treatment supervision. Here, we show with computer simulations that varying optical properties have a strong influence on the irradiation time required to fully bleach the photosensitizer. We propose a method to potentially determine the time point during iPDT, when the photosensitizer within the target volume has been largely photobleached. Simulations show that it is possible to determine this time point by continuously monitoring the ratio of the fluorescence intensities at two time points during irradiation. We show that this method works for a large range of optical properties, different photobleaching rates and varying inter-fibre distances. In conclusion, the relative fluorescence method offers the potential to individualize irradiation times to consume the photosensitizer within the target tissue during iPDT.

摘要

间质光动力疗法(iPDT)正被研究用于治疗高级别人类脑恶性肿瘤。在最近的临床研究中,荧光监测在多形性成胶质细胞瘤的 iPDT 中显示了光敏剂(氨基酮戊酸(ALA)诱导的原卟啉 IX,PpIX)及其光漂白动力学的患者特异性积累。由于光降解,也称为光漂白,以及组织损伤是由相同的潜在过程引起的,因此光漂白动力学可能提供实时治疗监测的工具。在这里,我们通过计算机模拟表明,光学性质的变化对完全漂白光敏剂所需的辐照时间有很大的影响。我们提出了一种潜在的方法来确定在 iPDT 期间的时间点,当目标体积内的光敏剂已经被大量光漂白时。模拟表明,通过在辐照过程中连续监测两个时间点的荧光强度比,可以确定这个时间点。我们表明,该方法适用于广泛的光学性质、不同的光漂白率和不同的纤维间距离。总之,相对荧光法有可能在 iPDT 中使目标组织内的光敏剂的辐照时间个体化。

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