题名 | RAB27B controls palmitoylation-dependent NRAS trafficking and signaling in myeloid leukemia |
作者 | |
通讯作者 | Tong,Wei |
发表日期 | 2023-06-15
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DOI | |
发表期刊 | |
ISSN | 0021-9738
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EISSN | 1558-8238
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卷号 | 133期号:12 |
摘要 | RAS mutations are among the most prevalent oncogenic drivers in cancers. RAS proteins propagate signals only when associated with cellular membranes as a consequence of lipid modifications that impact their trafficking. Here, we discovered that RAB27B, a RAB family small GTPase, controlled NRAS palmitoylation and trafficking to the plasma membrane, a localization required for activation. Our proteomic studies revealed RAB27B upregulation in CBL- or JAK2-mutated myeloid malignancies, and its expression correlated with poor prognosis in acute myeloid leukemias (AMLs). RAB27B depletion inhibited the growth of CBL-deficient or NRAS-mutant cell lines. Strikingly, Rab27b deficiency in mice abrogated mutant but not WT NRAS–mediated progenitor cell growth, ERK signaling, and NRAS palmitoylation. Further, Rab27b deficiency significantly reduced myelomonocytic leukemia development in vivo. Mechanistically, RAB27B interacted with ZDHHC9, a palmitoyl acyltransferase that modifies NRAS. By regulating palmitoylation, RAB27B controlled c-RAF/MEK/ERK signaling and affected leukemia development. Importantly, RAB27B depletion in primary human AMLs inhibited oncogenic NRAS signaling and leukemic growth. We further revealed a significant correlation between RAB27B expression and sensitivity to MEK inhibitors in AMLs. Thus, our studies presented a link between RAB proteins and fundamental aspects of RAS posttranslational modification and trafficking, highlighting future therapeutic strategies for RAS-driven cancers. |
相关链接 | [Scopus记录] |
收录类别 | |
语种 | 英语
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重要成果 | NI论文
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学校署名 | 其他
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资助项目 | National Institutes of Health[R01CA152108]
; National Institutes of Health[R01CA163489]
; National Institutes of Health[R01CA271523]
; National Institutes of Health[R01DK127738]
; National Institutes of Health[R35CA253178]
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WOS研究方向 | Research & Experimental Medicine
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WOS类目 | Medicine, Research & Experimental
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WOS记录号 | WOS:001022654700006
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出版者 | |
ESI学科分类 | CLINICAL MEDICINE
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Scopus记录号 | 2-s2.0-85161985387
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来源库 | Scopus
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引用统计 |
被引频次[WOS]:3
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成果类型 | 期刊论文 |
条目标识符 | http://sustech.caswiz.com/handle/2SGJ60CL/559936 |
专题 | 南方科技大学医学院_生物化学系 南方科技大学医学院 |
作者单位 | 1.State Key Laboratory Breeding Base of Basic Science of Stomatology (Hubei-MOST),Key Laboratory of Oral Biomedicine,Ministry of Education,School and Hospital of Stomatology,Wuhan University,Wuhan,Hubei,China 2.Division of Hematology,Children’s Hospital of Philadelphia,Philadelphia,United States 3.Department of Pediatrics,Perelman School of Medicine,The University of Pennsylvania,Philadelphia,United States 4.Department of Biochemistry,School of Medicine,The Southern University of Science and Technology,Shenzhen,Guangdong,China 5.Department of Medicine,Perlmutter Cancer Center,New York University Grossman School of Medicine,New York,United States 6.Department of Pathology,University of Utah,Salt Lake City,United States 7.Department of Biochemistry and Biophysics,Perelman School of Medicine,University of Pennsylvania,Philadelphia,United States 8.McArdle Laboratory for Cancer Research,University of Wisconsin–Madison,Madison,United States 9.Pathology and Laboratory Medicine,Children’s Hospital of Philadelphia,Philadelphia,United States 10.Division of Hematology and Oncology,Abramson Cancer Center,University of Pennsylvania,Philadelphia,United States |
推荐引用方式 GB/T 7714 |
Ren,Jian Gang,Xing,Bowen,Lv,Kaosheng,et al. RAB27B controls palmitoylation-dependent NRAS trafficking and signaling in myeloid leukemia[J]. Journal of Clinical Investigation,2023,133(12).
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APA |
Ren,Jian Gang.,Xing,Bowen.,Lv,Kaosheng.,O’Keefe,Rachel A..,Wu,Mengfang.,...&Tong,Wei.(2023).RAB27B controls palmitoylation-dependent NRAS trafficking and signaling in myeloid leukemia.Journal of Clinical Investigation,133(12).
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MLA |
Ren,Jian Gang,et al."RAB27B controls palmitoylation-dependent NRAS trafficking and signaling in myeloid leukemia".Journal of Clinical Investigation 133.12(2023).
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