Your search keyword '"Zhang, Yunkui"' showing total 2 results

1. Single-cell profiling of the microenvironment in human bone metastatic renal cell carcinoma.

Author

Ma, Fen, Wang, Shuoer, Xu, Lun, Huang, Wending, Shi, Guohai, Sun, Zhengwang, Cai, Weiluo, Wu, Zhiqiang, Huang, Yiming, Meng, Juan, Sun, Yining, Fang, Meng, Cheng, Mo, Ji, Yingzheng, Hu, Tu, Zhang, Yunkui, Gu, Bingxin, Zhang, Jiwei, Song, Shaoli, and Sun, Yidi

Subjects

RENAL cell carcinoma, MYELOID-derived suppressor cells, BONE marrow cancer, BONE metastasis, METASTASIS, BONE marrow, MOLECULAR pathology

Abstract

Bone metastasis is of common occurrence in renal cell carcinoma with poor prognosis, but no optimal treatment approach has been established for bone metastatic renal cell carcinoma. To explore the potential therapeutic targets for bone metastatic renal cell carcinoma, we profile single cell transcriptomes of 6 primary renal cell carcinoma and 9 bone metastatic renal cell carcinoma. We also include scRNA-seq data of early-stage renal cell carcinoma, late-stage renal cell carcinoma, normal kidneys and healthy bone marrow samples in the study to better understand the bone metastasis niche. The molecular properties and dynamic changes of major cell lineages in bone metastatic environment of renal cell carcinoma are characterized. Bone metastatic renal cell carcinoma is associated with multifaceted immune deficiency together with cancer-associated fibroblasts, specifically appearance of macrophages exhibiting malignant and pro-angiogenic features. We also reveal the dominance of immune inhibitory T cells in the bone metastatic renal cell carcinoma which can be partially restored by the treatment. Trajectory analysis showes that myeloid-derived suppressor cells are progenitors of macrophages in the bone metastatic renal cell carcinoma while monocytes are their progenitors in primary tumors and healthy bone marrows. Additionally, the infiltration of immune inhibitory CD47+ T cells is observed in bone metastatic tumors, which may be a result of reduced phagocytosis by SIRPA-expressing macrophages in the bone microenvironment. Together, our results provide a systematic view of various cell types in bone metastatic renal cell carcinoma and suggest avenues for therapeutic solutions. Single-cell profiling of primary and bone metastatic renal cell carcinoma suggests variation in intratumoral heterogeneity between samples and the is a valuable resource for examining the underlying pathogenic mechanisms for these cancers. [ABSTRACT FROM AUTHOR]

Published

2024

2. YTHDF1 promotes the osteolytic bone metastasis of breast cancer via inducing EZH2 and CDH11 translation.

Author

Wang, Shuoer, Xu, Lun, Wang, Dongliang, Zhao, Songjiao, Li, Kun, Ma, Fen, Yao, Qianlan, Zhang, Yunkui, Wu, Zhiqiang, Shao, Yang, Song, Shaoli, and Yan, Wangjun

Subjects

*METASTATIC breast cancer, *BONE metastasis, *STERNUM, *GENETIC translation, *MOLECULAR biology, *OSTEOBLASTS

Abstract

Bone metastasis is common in breast cancer and more effective therapies are required, however, its molecular mechanism is poorly understood. Additionally, the role of the m6A reader YTHDF1 in bone metastasis of breast cancer has not been reported. Here, we reveal that the increased expression of YTHDF1 is clinically correlated with breast cancer bone metastases. YTHDF1 promotes migration, invasion, and osteoblast adhesion and induces osteoclast differentiation of cancer cells in vitro and vivo. Mechanically, RNA-seq, MeRIP-seq and RIP-seq analysis, and molecular biology experiments demonstrate that YTHDF1 translationally enhances EZH2 and CDH11 expression by reading m6A-enriched sites of their transcripts. Moreover, adeno-associated virus (AAV) was used to deliver shYTHDF1 (shYTHDF1-AAV) in intratibial injection models, eliciting a significant suppressive effect on breast cancer bone metastatic formation and osteolytic destruction. Overall, we uncovered that YTHDF1 promotes osteolytic bone metastases of breast cancer by inducing EZH2 and CDH11 translation. • YTHDF1 overexpression clinically correlates with breast cancer bone metastases. • YTHDF1 promotes migration, invasion, osteoblast adhesion and induces osteoclast differentiation of breast cancer cells. • YTHDF1 promotes translation of the key bone metastatic genes EZH2 and CDH11. • ShYTHDF1-AAV potently inhibits breast cancer bone metastatic formation and osteolytic destruction. [ABSTRACT FROM AUTHOR]

Published

2024