Polyacrylic Acid-Coated LaB(6) Nanoparticles as Efficient Sensitizers for Binary Proton Therapy.

聚丙烯酸包覆的 LaB(6) 纳米粒子作为二元质子治疗的有效敏化剂

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作者:Ryabtseva Mariya S, Filimonova Marina V, Filimonov Alexander S, Soldatova Olga V, Shitova Anna A, Rybachuk Vitaly A, Volkova Irina K, Nikolaev Kirill A, Kosachenko Alexander O, Koryakin Sergei N, Petrunya Dmitry S, Kotelnikova Polina A, Shemyakov Alexander E, Kolmanovich Danil D, Popov Anton L, Tikhonowski Gleb V, Popov Anton A, Timakova Anna A, Kolobov Andrey V, Deyev Sergey M, Kabashin Andrei V, Zavestovskaya Irina N
Proton beam therapy (PBT) is a rapidly advancing modality of hadron therapy. The primary advantage of proton therapy lies in a unique depth-dose distribution characterized by the Bragg peak, which enables a highly targeted irradiation of the area limited to the tumor, while minimizing the impact on healthy tissues. However, a broader clinical adoption of the ion beam therapy is limited by both economic and radiobiological constraints. One of the possible ways to increase the relative biological effectiveness (RBE) of proton therapy involves the use of radiosensitizers. Background/Objectives: In this work, we investigated the efficacy of using colloidal solutions of lanthanum hexaboride (LaB(6)) nanoparticles (NPs) coated with polyacrylic acid (PAA) as sensitizers to increase the antitumor biological effectiveness of proton irradiation. This material has not yet been studied extensively so far, despite its promising physical and chemical properties and several reports on its biocompatibility. Methods: LaB(6) NPs were synthesized by femtosecond pulsed laser ablation, functionalized with PAA and characterized. The safety of NPs was evaluated in vitro using a Live/Dead assay on cell cultures: EMT6/P, BT-474, and in vivo in Balb/c mice after intravenous (i.v.) administration. The efficacy of binary proton therapy was evaluated in vitro on cell cultures: EMT6/P, BT-474, and in vivo in the model of human ductal carcinoma of the mammary gland BT-474 in female Nu/j mice after intratumoral (i.t.) administration at a dose of 2.0 mg/mouse and local proton irradiation (fractional exposure of 31 Gy + 15 Gy). The biodistribution of LaB(6)-PAA NPs in the animal body was also evaluated. Results: Significant enhancement in cancer cell death following proton beam irradiation was demonstrated in vitro on EMT6/P, BT-474 cell lines. Although the antitumor efficacy observed in vivo was comparatively lower-likely due to the high sensitivity of the BT-474 xenografts-both proton monotherapy and binary treatment were well tolerated. Conclusions: LaB(6)-PAA NPs show promise as efficient sensitizers capable of enhancing the biological efficacy of proton therapy, offering a potential path forward for improving therapeutic outcomes.

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