Insights into the osteosarcoma microenvironment: Multiscale analysis of structural and mineral heterogeneity.

Francesca Rossi, Martyna Malgorzata Rydzyk, Luisa Barba, Emil Malucelli, Maria Elisabetta Federica Palamà, Chiara Gentili, Maddalena Mastrogiacomo, Alessia Cedola, Lucia Mancini, Murielle Salomé, Hiram Castillo-Michel, Davide Maria Donati, Marco Gambarotti, Enrico Lucarelli, Michela Fratini, Stefano Iotti
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Abstract

Osteosarcoma (OS) is a malignant and heterogeneous disease that typically originates in the long bones of children and adolescents. It is characterized by the presence of immature cells having an aggressive phenotype and rapid uncontrolled proliferation. OS progression induces significant molecular and cellular changes locally within the bone, resulting in the development of an abnormal tumor microenvironment (TME). The OS TME plays a crucial role in tumor progression and development, however, the precise effects of OS on bone structure and mineralization still remain poorly understood. In this study, we examined the OS TME by analyzing samples from osteoblastic, parosteal, and periosteal osteosarcomas. Employing advanced synchrotron-based X-ray techniques, we performed a multiscale analysis to evaluate the structural and mineral complexity of tumor-affected bone. Our results revealed marked morphological differences among the osteosarcoma subtypes, while confirming that biomineralization remains active through the production of hydroxyapatite (HA). X-ray diffraction identified two distinct hydroxyapatite crystalline phases across all samples, suggesting a critical behavior of minerals in bone. Additionally, we observed that the bone mineral structure in periosteal and parosteal osteosarcomas exhibited crystal deformations along the c-axis, whereas the osteoblastic osteosarcoma displayed a mineral profile comparable to control bone. Micro-X-ray absorption near-edge spectroscopy revealed the occurrence of a dysregulated biomineralization in the parosteal and periosteal subtypes, marked by the presence of calcium compounds different from HA, in contrast to the mature mineral state found in the osteoblastic variant. These findings highlight the complexity of osteosarcoma repercussion on bone tissue, offering new insights into the interactions within the OS TME. STATEMENT OF SIGNIFICANCE: This study investigates the tumor microenvironment (TME) of osteosarcoma (OS), a rare and aggressive bone cancer mainly affecting children and adolescents. Using advanced synchrotron-based X-ray techniques, we analyzed structural and mineral alterations in bone from three OS subtypes: osteoblastic, parosteal, and periosteal. The results reveal distinct subtype-specific differences in bone mineralization and crystallinity, highlighting the heterogeneity of OS and the pivotal role of its microenvironment in driving disease progression. This research contributes to our understanding of OS pathophysiology and provides foundation for future studies aimed at developing targeted therapies and improving diagnostic approaches.

洞察骨肉瘤微环境:结构和矿物异质性的多尺度分析。
骨肉瘤(OS)是一种恶性和异质性疾病,通常起源于儿童和青少年的长骨。它的特点是存在具有侵略性表型和快速不受控制的增殖的未成熟细胞。骨肉瘤的进展在骨内局部诱导显著的分子和细胞变化,导致异常肿瘤微环境(TME)的发展。骨肉瘤TME在肿瘤进展和发展中起着至关重要的作用,然而,骨肉瘤对骨结构和矿化的确切影响仍然知之甚少。在这项研究中,我们通过分析成骨细胞、骨旁和骨膜骨肉瘤的样本来检查OS TME。采用先进的基于同步加速器的x射线技术,我们进行了多尺度分析,以评估受肿瘤影响的骨骼的结构和矿物复杂性。我们的研究结果揭示了骨肉瘤亚型之间的显著形态差异,同时证实了生物矿化通过产生羟基磷灰石(HA)保持活跃。x射线衍射在所有样品中鉴定出两种不同的羟基磷灰石结晶相,表明骨骼中矿物质的关键行为。此外,我们观察到骨膜骨肉瘤和骨旁骨肉瘤的骨矿物结构沿c轴呈晶体变形,而成骨细胞骨肉瘤的矿物结构与对照骨相当。微x射线吸收近边光谱揭示了骨旁和骨膜亚型中生物矿化失调的发生,其特征是存在不同于透明质酸的钙化合物,与成骨细胞变体中发现的成熟矿物状态形成对比。这些发现突出了骨肉瘤对骨组织的影响的复杂性,为OS TME内的相互作用提供了新的见解。意义声明:本研究探讨骨肉瘤(osteosarcoma, OS)的肿瘤微环境(tumor microenvironment, TME),这是一种主要影响儿童和青少年的罕见侵袭性骨癌。使用先进的基于同步加速器的x射线技术,我们分析了三种骨肉瘤亚型骨的结构和矿物变化:成骨细胞、骨旁和骨膜。结果揭示了骨矿化和结晶度的不同亚型特异性差异,突出了骨肉瘤的异质性及其微环境在驱动疾病进展中的关键作用。本研究有助于我们对OS病理生理学的理解,并为未来的研究提供基础,旨在开发靶向治疗和改进诊断方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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