Integrated Microbiome and Metabolome Analysis Reveals Hypothalamic‐Comorbidities Related Signatures in Craniopharyngioma

Author:

Lin Ben1,Ye Zhen1,Cao Zhan23,Ye Zhao1,Yu Yifei4,Jiang Weiliang56,Guo Sichen7,Melnikov Vladimir4,Zhou Peng8,Ji Chenxing1,Shi Chengzhang1,Wu Zerui1,Chen Zhengyuan1,Xu Yihua1,Zhang Qilin1,Ma Zengyi1,Qiao Nidan1,Chen Long1,Shou Xuefei1,Cao Xiaoyun1,Zhou Xiang1,Zhang Li4,He Min4,Wang Yongfei1,Ye Hongying4,Li Yiming4,Zhang Zhaoyun4,Wang Meng4,Gao Renyuan2,Zhang Yichao19101112ORCID

Affiliation:

1. Department of Neurosurgery Huashan Hospital Fudan University Shanghai 200040 China

2. Department of General Surgery Shanghai Tenth People's Hospital School of Medicine Tongji University Shanghai 200072 China

3. Institute of Gut Microbiota Research and Engineering Development Shanghai Tenth People's Hospital Tongji University School of Medicine Shanghai 200072 China

4. Department of Endocrinology and Metabolism Huashan Hospital Fudan University Shanghai 200040 China

5. Department of Gastroenterology Shanghai General Hospital Shanghai Jiao Tong University School of Medicine Shanghai 200080 China

6. Shanghai Key Laboratory of Pancreatic Disease Institute of Pancreatic Disease, Shanghai Jiao Tong University School of Medicine Shanghai 201620 China

7. Shanghai Medical College Fudan University Shanghai 200032 China

8. Department of Cardiology Huashan Hospital Fudan University Shanghai 200040 China

9. National Center for Neurological Disorders Shanghai 200040 China

10. Shanghai Key Laboratory of Brain Function and Restoration and Neural Regeneration Shanghai 200040 China

11. Neurosurgical Institute of Fudan University Fudan University Shanghai 200040 China

12. Shanghai Clinical Medical Center of Neurosurgery Shanghai 200040 China

Abstract

AbstractCraniopharyngioma (CP) is an intracranial tumor with high mortality and morbidity. Though biologically benign, CP will damage the hypothalamus, inducing comorbidities such as obesity, metabolic syndrome, and cognitive impairments. The roles of gut microbiome and serum metabolome in CP‐associated hypothalamic comorbidities are aimed to be explored. Patients with CP are characterized by increased Shannon diversity, Eubacterium, Clostridium, and Roseburia, alongside decreased Alistipes and Bacteroides. CP‐enriched taxa are positively correlated with dyslipidemia and cognitive decline, while CP‐depleted taxa are negatively associated with fatty liver. Subsequent serum metabolomics identified notably up‐regulated purine metabolism, and integrative analysis indicated an association between altered microbiota and elevated hypoxanthine. Phenotypic study and multi‐omics analysis in the Rax‐CreERT2::BrafV600E/+::PtenFlox/+ mouse model validated potential involvement of increased Clostridium and dysregulated purine metabolism in hypothalamic comorbidities. To further consolidate this, intervention experiments are performed and it is found that hypoxanthine co‐variated with the severity of hypothalamic comorbidities and abundance of Clostridium, and induced dysregulated purine metabolism along with redox imbalance in target organs (liver and brain cortex). Overall, the study demonstrated the potential of increased Clostridium and up‐regulated purine metabolism as signatures of CP‐associated hypothalamic‐comorbidities, and unveiled that elevated Clostridium, dysregulated purine metabolism, and redox imbalance may mediate the development and progression of CP‐associated hypothalamic‐comorbidities.

Funder

National Natural Science Foundation of China

Shanghai Science and Technology Development Foundation

Natural Science Foundation of Shanghai Municipality

Publisher

Wiley

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