Elucidation of the Catalytic Apparatus and Mechanism of Human Chitotriosidase-1

IF 13.1 1区化学 Q1 CHEMISTRY, PHYSICAL

ACS Catalysis Pub Date : 2025-09-19 DOI:10.1021/acscatal.5c00507

Dorota Niedzialek*, , , Grzegorz Wieczorek, , , Katarzyna Drzewicka, , , Anna Antosiewicz, , , Mariusz Milewski, , , Agnieszka Bartoszewicz, , , Jacek Olczak*, , and , Zbigniew Zasłona*,

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引用次数: 0

Abstract

Despite extensive research over the past three decades, the catalytic mechanism of human chitotriosidase-1 (hCHIT1) has remained incompletely understood. To address this gap, we reanalyzed all available structural information and, integrating experimental data with multiscale molecular simulations, successfully modeled the full-length structure of hCHIT1 for the first time, including the previously unresolved proline-rich linker essential for domain communication. This comprehensive model enabled us to propose a general mechanism of hCHIT1 catalysis and to elucidate the distinct functional roles of all four highly conserved structural motifs of the glycoside hydrolase 18 (GH18) family, a group comprising over 65,000 known members across all domains of life. We further investigated the influence of monovalent metal ions in achieving optimal catalytic conditions and determined the activation energies for both substrate-assisted hydrolysis and transglycosylation processes. Our simulations revealed coordinated Brownian conformational fluctuations within hCHIT1 subdomains, which collectively harness thermal energy to drive catalysis. Notably, we discovered a previously unreported piston-like mechanism in which a conserved tyrosine residue transduces mechanical energy to the substrate, significantly lowering the activation barrier for catalysis. Additionally, by constructing a complete substrate model, we resolved the long-standing mechanistic enigma of the highly conserved tryptophan ‘lid’ at the active site entrance, demonstrating its multifaceted role in substrate gating, transition state stabilization, and product release. Finally, we demonstrated that binding of the first-in-class inhibitor OATD-01 induces subtle yet far-reaching dynamical changes within the active site, leading to dissociation of the immunoglobulin-like heterodimer and disruption of interactions with biological partners implicated in disease pathogenesis. These findings not only redefine the mechanistic landscape of hCHIT1 but also provide a robust framework for the rational design of next-generation GH18 inhibitors, for example, targeting multidrug-resistant pathogens.

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人壳三酸苷酶-1催化装置及机理的研究

尽管在过去的三十年中进行了广泛的研究，但人类壳三酸苷酶-1 （hCHIT1）的催化机制仍然不完全清楚。为了解决这一差距，我们重新分析了所有可用的结构信息，并将实验数据与多尺度分子模拟相结合，首次成功地模拟了hCHIT1的全长结构，包括以前未解决的富含脯氨酸的连接子，这是结构域通信所必需的。这个综合模型使我们能够提出hCHIT1催化的一般机制，并阐明糖苷水解酶18 （GH18）家族中所有四个高度保守的结构基元的不同功能作用，该家族包括65,000多个已知成员，分布在所有生命领域。我们进一步研究了单价金属离子对获得最佳催化条件的影响，并确定了底物辅助水解和转糖基化过程的活化能。我们的模拟揭示了hCHIT1亚域内协调的布朗构象波动，它们共同利用热能驱动催化。值得注意的是，我们发现了一种以前未报道过的类似活塞的机制，其中一个保守的酪氨酸残基将机械能传递给底物，显著降低了催化的激活屏障。此外，通过构建一个完整的底物模型，我们解决了活性位点入口高度保守的色氨酸“盖子”的长期机制之谜，证明了它在底物控制、过渡态稳定和产物释放方面的多方面作用。最后，我们证明了一流抑制剂OATD-01的结合在活性部位诱导了微妙但深远的动态变化，导致免疫球蛋白样异二聚体的解离，并破坏了与疾病发病机制相关的生物伴侣的相互作用。这些发现不仅重新定义了hCHIT1的机制景观，而且为合理设计下一代GH18抑制剂（例如针对多药耐药病原体）提供了强有力的框架。

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来源期刊

ACS Catalysis CHEMISTRY, PHYSICAL-

CiteScore

20.80

自引率

6.20%

发文量

1253

审稿时长

1.5 months

期刊介绍： ACS Catalysis is an esteemed journal that publishes original research in the fields of heterogeneous catalysis, molecular catalysis, and biocatalysis. It offers broad coverage across diverse areas such as life sciences, organometallics and synthesis, photochemistry and electrochemistry, drug discovery and synthesis, materials science, environmental protection, polymer discovery and synthesis, and energy and fuels. The scope of the journal is to showcase innovative work in various aspects of catalysis. This includes new reactions and novel synthetic approaches utilizing known catalysts, the discovery or modification of new catalysts, elucidation of catalytic mechanisms through cutting-edge investigations, practical enhancements of existing processes, as well as conceptual advances in the field. Contributions to ACS Catalysis can encompass both experimental and theoretical research focused on catalytic molecules, macromolecules, and materials that exhibit catalytic turnover.