【第64期】前沿靶點速遞:每周醫(yī)學研究精選
日期:2025-11-18 16:30:47
01、靶點:SKP2、STUB1
應用:腫瘤免疫治療
來源:A rapid imaging-based screen for induced-proximity degraders identifies a potent degrader of oncoprotein SKP2.Nat Biotechnol,2025 Sep 10
02、靶點:Munc13-4
應用:腫瘤免疫治療
來源:Munc13-4 mediates tumor immune evasion by regulating the sorting and secretion of PD-L1 via exosomes.Nat Commun,2025 Oct 13
2025年10月13日,華中科技大學馬聰教授團隊聯(lián)合中國科學院廣州生物醫(yī)藥與健康研究院何俊教授團隊在《Nature Communications》發(fā)表研究論文,揭示了Munc13-4通過調(diào)控外泌體PD-L1的分選與分泌促進腫瘤免疫逃逸的新機制。研究發(fā)現(xiàn),Munc13-4在多種腫瘤組織中表達上調(diào),其缺失可增強T細胞介導的抗腫瘤反應。Munc13-4通過與PD-L1結(jié)合并招募HRS形成三元復合物,調(diào)控PD-L1的分選,并協(xié)同Rab27a介導多囊泡體錨定至細胞膜,促進外泌體分泌。干擾素γ通過調(diào)控Munc13-4與HRS的修飾動態(tài)控制PD-L1分選。基于此,團隊開發(fā)了靶向Munc13-4與PD-L1互作的小肽P-pep,可阻斷PD-L1進入外泌體,顯著增強腫瘤微環(huán)境中T細胞的浸潤與活化,抑制腫瘤生長,為免疫治療提供了新策略。
03、靶點:BRRF2
應用:EBV相關腫瘤免疫治療
來源:Extracellular vesicles derived EBV tegument protein BRRF2 suppresses cGAS phase separation to promote anti-viral innate immune evasion.Nat Commun,2025 Oct 10
04、靶點:RAB22A
應用:結(jié)直腸癌的治療
來源:RAB22A triggers intercellular chemoresistance transmission in colorectal cancer by promoting exosome release via the PKM2-pSNAP23 axis.Oncogene,2025 Nov
05、靶點:USP2
應用:MASLD的治療
來源:USP2 promotes metabolic dysfunction-associated steatotic liver disease progression via stabilization of PPARγ.Cell Death Differ,2025 Sep 24
06、靶點:PFKL
應用:解決實體瘤耐藥問題
來源:The noncanonical function of liver-type
phosphofructokinase potentiates the efficacy of HDAC inhibitors in cancer.Signal Transduct Target Ther,2025 Oct 14
推薦產(chǎn)品
參考文獻
[1]A rapid imaging-based screen for induced-proximity degraders identifies a potent degrader of oncoprotein SKP2.Nat Biotechnol,2025 Sep 10
[2]Munc13-4 mediates tumor immune evasion by regulating the sorting and secretion of PD-L1 via exosomes.Nat Commun,2025 Oct 13
[3]Extracellular vesicles derived EBV tegument protein BRRF2 suppresses cGAS phase separation to promote anti-viral innate immune evasion.Nat Commun,2025 Oct 10
[4]RAB22A triggers intercellular chemoresistance transmission in colorectal cancer by promoting exosome release via the PKM2-pSNAP23 axis.Oncogene,2025 Nov
[5]USP2 promotes metabolic dysfunction-associated steatotic liver disease progression via stabilization of PPARγ.Cell Death Differ,2025 Sep 24
[6]The noncanonical function of liver-type phosphofructokinase potentiates the efficacy of HDAC inhibitors in cancer.Signal Transduct Target Ther,2025 Oct 14
*免責聲明:華美生物內(nèi)容團隊僅是分享和解讀公開研究論文及其發(fā)現(xiàn),本文僅作信息交流,文中觀點不代表華美生物立場,請理解。
應用:腫瘤免疫治療
來源:A rapid imaging-based screen for induced-proximity degraders identifies a potent degrader of oncoprotein SKP2.Nat Biotechnol,2025 Sep 10
圖源:10.1038/s41587-025-02793-8[1]
2025年9月10日,廈門大學鄧賢明團隊與中國科學院分子細胞科學卓越創(chuàng)新中心姜海團隊在《Nature Biotechnology》發(fā)表研究論文,構(gòu)建了基于“死亡-存活”表型轉(zhuǎn)換的高通量蛋白降解劑篩選體系DEFUSE,并發(fā)現(xiàn)新型分子膠降解劑SKPer1。SKPer1通過泛素連接酶STUB1高效降解腫瘤驅(qū)動蛋白SKP2,展現(xiàn)出顯著抗腫瘤活性。該研究突破了“不可成藥”靶點SKP2的治療瓶頸,為分子膠降解劑的系統(tǒng)性篩選提供了全新技術路徑,還拓展了分子膠技術體系,具有重要意義。02、靶點:Munc13-4
應用:腫瘤免疫治療
來源:Munc13-4 mediates tumor immune evasion by regulating the sorting and secretion of PD-L1 via exosomes.Nat Commun,2025 Oct 13
圖源:10.1038/s41467-025-64149-9[2]
2025年10月13日,華中科技大學馬聰教授團隊聯(lián)合中國科學院廣州生物醫(yī)藥與健康研究院何俊教授團隊在《Nature Communications》發(fā)表研究論文,揭示了Munc13-4通過調(diào)控外泌體PD-L1的分選與分泌促進腫瘤免疫逃逸的新機制。研究發(fā)現(xiàn),Munc13-4在多種腫瘤組織中表達上調(diào),其缺失可增強T細胞介導的抗腫瘤反應。Munc13-4通過與PD-L1結(jié)合并招募HRS形成三元復合物,調(diào)控PD-L1的分選,并協(xié)同Rab27a介導多囊泡體錨定至細胞膜,促進外泌體分泌。干擾素γ通過調(diào)控Munc13-4與HRS的修飾動態(tài)控制PD-L1分選。基于此,團隊開發(fā)了靶向Munc13-4與PD-L1互作的小肽P-pep,可阻斷PD-L1進入外泌體,顯著增強腫瘤微環(huán)境中T細胞的浸潤與活化,抑制腫瘤生長,為免疫治療提供了新策略。
03、靶點:BRRF2
應用:EBV相關腫瘤免疫治療
來源:Extracellular vesicles derived EBV tegument protein BRRF2 suppresses cGAS phase separation to promote anti-viral innate immune evasion.Nat Commun,2025 Oct 10
圖源:10.1038/s41467-025-64037-2[3]
2025年10月10日,中山大學腫瘤防治中心鐘茜、曾木圣研究團隊在《Nature Communications》發(fā)表研究,揭示EB病毒(EBV)通過細胞外囊泡(EVs)遞送BRRF2蛋白,破壞宿主天然免疫防線,助力腫瘤免疫逃逸。EBV是與多種癌癥相關的人類致癌病毒,其在鼻咽癌等腫瘤中通過EVs將BRRF2精準遞送至巨噬細胞。BRRF2通過與cGAS蛋白特異性結(jié)合,阻斷DNA識別、瓦解相分離、抑制酶活性,癱瘓cGAS-STING信號通路,抑制抗病毒免疫應答。此外,BRRF2還促進EBV復制,形成“免疫逃逸-病毒復制”的正反饋環(huán)路。該研究為克服EBV相關腫瘤免疫治療抵抗提供了新方向。04、靶點:RAB22A
應用:結(jié)直腸癌的治療
來源:RAB22A triggers intercellular chemoresistance transmission in colorectal cancer by promoting exosome release via the PKM2-pSNAP23 axis.Oncogene,2025 Nov
圖源:10.1038/s41388-025-03566-y[4]
江南大學附屬醫(yī)院腫瘤研究所黃朝暉教授/殷媛研究員團隊在《Oncogene》發(fā)表研究,揭示外泌體介導結(jié)直腸癌化療耐藥的新機制。研究發(fā)現(xiàn),小G蛋白RAB22A不僅直接促進結(jié)直腸癌細胞化療耐藥,還通過促進富含RAB22A-PKM2的外泌體分泌,誘導腫瘤微環(huán)境中其他癌細胞獲得性耐藥。RAB22A通過抑制PKM2的泛素化和降解,促進SNAP-23的磷酸化,增加外泌體分泌。耐藥細胞分泌的外泌體攜帶RAB22A和穩(wěn)定PKM2,被敏感細胞吞噬后,增強其耐藥能力。該研究為結(jié)直腸癌化療耐藥的精準預測和靶向逆轉(zhuǎn)提供了新策略。05、靶點:USP2
應用:MASLD的治療
來源:USP2 promotes metabolic dysfunction-associated steatotic liver disease progression via stabilization of PPARγ.Cell Death Differ,2025 Sep 24
圖源:10.1038/s41418-025-01589-2[5]
上海交通大學醫(yī)學院吳英理課題組在《Cell Death & Differentiation》發(fā)表研究,揭示去泛素化酶USP2通過穩(wěn)定PPARγ促進代謝功能障礙相關脂肪性肝病(MASLD)的進展。研究發(fā)現(xiàn),USP2在MASLD肝臟組織中表達上調(diào),其特異性去除PPARγ DNA結(jié)合域中第161位賴氨酸上的K48連接的多聚泛素鏈,阻止PPARγ被蛋白酶體降解,增強其穩(wěn)定性和轉(zhuǎn)錄活性,促進脂質(zhì)合成相關基因表達,導致肝細胞脂質(zhì)蓄積。團隊利用肝靶向GalNAc-siRNA技術驗證了USP2作為治療靶點的潛力,為MASLD的治療提供了新策略。06、靶點:PFKL
應用:解決實體瘤耐藥問題
來源:The noncanonical function of liver-type
phosphofructokinase potentiates the efficacy of HDAC inhibitors in cancer.Signal Transduct Target Ther,2025 Oct 14
圖源:10.1038/s41392-025-02443-0[6]
10月14日,海軍軍醫(yī)大學王紅陽院士/董立巍研究員團隊在《Signal Transduction and Targeted Therapy》(IF=52.7)發(fā)表成果,揭示肝型磷酸果糖激酶(PFKL)是提升組蛋白去乙酰化酶抑制劑(HDACi)實體瘤療效的關鍵因子。研究以膽管癌為模型,發(fā)現(xiàn)PFKL在細胞核中調(diào)控HDACi療效和細胞內(nèi)表觀遺傳動力學。基于此,團隊開發(fā)了一種細胞穿透性治療肽,利用PFKL增強藥物精準性,顯著提升抗腫瘤效果,為解決實體瘤耐藥問題提供新策略。推薦產(chǎn)品
| 靶點 | 重組蛋白 | 貨號 |
| BRRF2 | Recombinant Epstein-Barr virus Tegument protein BRRF2 (BRRF2), partial | CSB-MP365877EFA |
| PFKL | Recombinant Human ATP-dependent 6-phosphofructokinase, liver type (PFKL) | CSB-MP017821HU |
| RAB22A | Recombinant Human Ras-related protein Rab-22A (RAB22A) | CSB-MP891957HU |
| SKP2 | Recombinant Human S-phase kinase-associated protein 2 (SKP2) | CSB-EP613392HU |
| STUB1 | Recombinant Human E3 ubiquitin-protein ligase CHIP (STUB1) | CSB-EP892480HUe1 |
| UNC13D | Recombinant Human Protein unc-13 homolog D (UNC13D), partial | CSB-MP758222HU |
| USP2 | Recombinant Human Ubiquitin carboxyl-terminal hydrolase 2 (USP2) | CSB-MP025710HU |
參考文獻
[1]A rapid imaging-based screen for induced-proximity degraders identifies a potent degrader of oncoprotein SKP2.Nat Biotechnol,2025 Sep 10
[2]Munc13-4 mediates tumor immune evasion by regulating the sorting and secretion of PD-L1 via exosomes.Nat Commun,2025 Oct 13
[3]Extracellular vesicles derived EBV tegument protein BRRF2 suppresses cGAS phase separation to promote anti-viral innate immune evasion.Nat Commun,2025 Oct 10
[4]RAB22A triggers intercellular chemoresistance transmission in colorectal cancer by promoting exosome release via the PKM2-pSNAP23 axis.Oncogene,2025 Nov
[5]USP2 promotes metabolic dysfunction-associated steatotic liver disease progression via stabilization of PPARγ.Cell Death Differ,2025 Sep 24
[6]The noncanonical function of liver-type phosphofructokinase potentiates the efficacy of HDAC inhibitors in cancer.Signal Transduct Target Ther,2025 Oct 14
*免責聲明:華美生物內(nèi)容團隊僅是分享和解讀公開研究論文及其發(fā)現(xiàn),本文僅作信息交流,文中觀點不代表華美生物立場,請理解。
