Gut microbiota deficiency ameliorates multiple myeloma and myeloma-related bone disease by Th17 cells in mice models

Liu, Jia; Xie, Fang; Yi, Zhi-gang; Ma, Tao; Tie, Wen-ting; Li, Yan-hong; Bai, Jun; Zhang, Lian-sheng

doi:10.7150/jca.88799

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International Journal of Biological Sciences

International Journal of Medical Sciences

Theranostics

Journal of Genomics

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J Cancer 2023; 14(17):3191-3202. doi:10.7150/jca.88799 This issue Cite

Research Paper

Gut microbiota deficiency ameliorates multiple myeloma and myeloma-related bone disease by Th17 cells in mice models

Jia Liu, Fang Xie, Zhi-gang Yi, Tao Ma, Wen-ting Tie, Yan-hong Li, Jun Bai, Lian-sheng Zhang^✉

Department of Hematology, Lanzhou University Second Hospital, Lanzhou 730000, China.

Citation:

Liu J, Xie F, Yi Zg, Ma T, Tie Wt, Li Yh, Bai J, Zhang Ls. Gut microbiota deficiency ameliorates multiple myeloma and myeloma-related bone disease by Th17 cells in mice models. J Cancer 2023; 14(17):3191-3202. doi:10.7150/jca.88799. https://www.jcancer.org/v14p3191.htm

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Abstract

Purpose: Multiple myeloma, the second most common hematological tumor, is currently incurable. Multiple myeloma-related bone disease is a characteristic clinical symptom that seriously affects the survival and prognosis of patients. In recent years, gut microbiota has been shown to play an important role in the occurrence and development of multiple myeloma. However, whether and how it affects the development of myelomatous bone disease is unclear.

Methods: To investigate the mechanism and influence of the microbiota on multiple myeloma and myeloma bone disease, a myeloma-gut microbiota deletion mice model was established. 16S rRNA sequencing was used to analysis of bacterial flora changes. Histochemical staining and bone micro-CT were used to assess the severity of bone disease. Bone marrow tumor load and spleen Th17 cells were detected by flow cytometry.

Results: Histochemical staining revealed a reduced tumor burden after eliminating gut microbial communities in mice by administering a mixture of antibiotics. According to the 16S rRNA sequencing of intestinal contents, antibiotic treatment resulted in a significant change in the microbiota of the mice. Bone micro-CT demonstrated that antibiotic treatment could reduce bone lesions caused by myeloma while increasing mineral density, bone volume fraction, trabecular bone thickness, and trabecular number. Meanwhile, histochemical staining of the bone found that the enhanced bone resorption was weakened by the change of flora. These results were consistent with the concentration of IL17 in serum and the frequency of Th17 cells in spleen.

Conclusions: Herein, the effects of the gut microbiome on myeloma bone disease are investigated for the first time, providing new insight into its pathogenesis and suggesting that gut microbiota may serve as a therapeutic target in multiple myeloma-associated bone diseases.

Keywords: Multiple myeloma, Multiple myeloma bone disease, Gut microbiome, 16S rRNA sequencing, IL-17/Th17 cell, Bone resorption

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APA

Liu, J., Xie, F., Yi, Z.g., Ma, T., Tie, W.t., Li, Y.h., Bai, J., Zhang, L.s. (2023). Gut microbiota deficiency ameliorates multiple myeloma and myeloma-related bone disease by Th17 cells in mice models. Journal of Cancer, 14(17), 3191-3202. https://doi.org/10.7150/jca.88799.

ACS

Liu, J.; Xie, F.; Yi, Z.g.; Ma, T.; Tie, W.t.; Li, Y.h.; Bai, J.; Zhang, L.s. Gut microbiota deficiency ameliorates multiple myeloma and myeloma-related bone disease by Th17 cells in mice models. J. Cancer 2023, 14 (17), 3191-3202. DOI: 10.7150/jca.88799.

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CSE

Liu J, Xie F, Yi Zg, Ma T, Tie Wt, Li Yh, Bai J, Zhang Ls. 2023. Gut microbiota deficiency ameliorates multiple myeloma and myeloma-related bone disease by Th17 cells in mice models. J Cancer. 14(17):3191-3202.

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