Natural Affinity Driven Modification by Silicene to Construct a “Thermal Switch” for Tumorous Bone Loss

Author:

Chen Yi‐Xing1,Luo Yi‐Ping1,Hou Xiao‐Dong1,Zhang Lei1,Wang Tian‐Long1,Li Xi‐Fan1,Liu Zhi‐Qing1,Zhao Jin‐Hui1,Aierken Aihemaitijiang1,Cai Zhu‐Yun2,Lu Bing‐Qiang1,Tan Shuo1,Zhao Xin‐Yu1,Chen Feng13,Zhou Zi‐Fei1,Zheng Long‐Po14ORCID

Affiliation:

1. Department of Orthopedics Shanghai Tenth People's Hospital School of Medicine Tongji University Shanghai 200072 China

2. Department of Orthopedics Second Affiliated Hospital of Naval Medical University 415 Fengyang Road Shanghai 200003 P. R. China

3. Shanghai Key Laboratory of Craniomaxillofacial Development and Diseases Shanghai Stomatological Hospital & School of Stomatology Fudan University Shanghai 201102 P. R. China

4. Shanghai Tenth People's Hospital Chongming Branch Shanghai 202150 China

Abstract

AbstractTumorous bone defects present significant challenges for surgical bio‐reconstruction due to the dual pathological conditions of residual tumor presence and extensive bone loss following excision surgery. To address this challenge, a “thermal switch” smart bone scaffold based on the silicene nanosheet‐modified decalcified bone matrix (SNS@DBM) is developed by leveraging the natural affinity between collagen and silicene, which is elucidated by molecular dynamics simulations. Benefitting from its exceptional photothermal ability, biodegradability, and bioactivity, the SNS@DBM “thermal switch” provides an integrated postoperative sequential thermotherapy for tumorous bone loss by exerting three levels of photothermal stimulation (i.e., strong, moderate, and nonstimulation). During the different phases of postoperative bioconstruction, the SNS@DBM scaffold realizes simultaneous residual tumor ablation, tumor recurrence prevention, and bone tissue regeneration. These biological effects are verified in the tumor‐bearing nude mice of patient‐derived tissue xenografts and critical cranium defect rats. Mechanism research prompts moderate heat stimulus generated by and coordinating with SNSs can upregulate osteogenic genes, promote macrophages M2 polarization, and intensify angiogenesis of H‐type vessels. This study introduces a versatile approach to the management of tumorous bone defects.

Funder

National Natural Science Foundation of China

National Key Research and Development Program of China

Natural Science Foundation of Shanghai Municipality

Publisher

Wiley

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