Albumin-binding photosensitizer capable of targeting glioma via the SPARC pathway

Author:

Li Xingshu1,Oh Jae Sang2,Lee Yoonji3,Lee Eun Chae2,Yang Mengyao4,Kwon Nahyun4,Ha Tae Won2,Hong Dong-Yong2,Song Yena2,Kim Hyun Kyu2,Song Byung Hoo2,Choi Sun4,Yoon Juyoung4ORCID,Lee Man Ryul2

Affiliation:

1. Fuzhou University

2. Soonchunhyang University

3. Chung-Ang University

4. Ewha Womans University

Abstract

Abstract Background Malignant glioma is among the most lethal and frequently occurring brain tumors, and the average survival period is 15 months. Existing chemotherapy has low tolerance and low blood-brain barrier (BBB) permeability; therefore, the required drug dose cannot be accurately delivered to the tumor site, resulting in an insufficient drug effect. Methods Herein, we demonstrate a precision photodynamic tumor therapy using a photosensitizer (ZnPcS) capable of binding to albumin in situ, which can increase the permeability of the BBB and accurately target glioma. Albumin-binding ZnPcS was designed to pass through the BBB and bind to secreted protein acidic and rich in cysteine (SPARC), which is abundant in the glioma plasma membrane. Results When the upper part of a mouse brain was irradiated using a laser (0.2 W cm− 2) after transplantation of glioma and injection of ZnPcS, tumor growth was inhibited by approximately 83.6%, and the 50% survival rate of the treatment group increased by 14 days compared to the control group. In glioma with knockout SPARC, the amount of ZnPcS entering the glioma was reduced by 63.1%, indicating that it can target glioma through the SPARC pathway. Conclusions This study showed that using albumin-binding photosensitizers is promising for the treatment of malignant gliomas.

Publisher

Research Square Platform LLC

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