協(xié)和麒麟宣布����,惠爾金?(莫格利珠單抗)已獲國家藥品監(jiān)督管理局(NMPA)的正式批準(zhǔn)�����,用于治療既往接受過系統(tǒng)性治療的復(fù)發(fā)或難治性塞扎里綜合征(SS)或晚期(III/IV)蕈樣肉芽腫(MF)成人患者��。
協(xié)和麒麟宣布�,惠爾金®(莫格利珠單抗)已獲國家藥品監(jiān)督管理局(NMPA)的正式批準(zhǔn),用于治療既往接受過系統(tǒng)性治療的復(fù)發(fā)或難治性塞扎里綜合征(SS)或晚期(III/IV)蕈樣肉芽腫(MF)成人患者[2]�。惠爾金®是中國首 個(gè)也是唯一獲批用于治療SS和MF的靶向CCR4的生物制劑[1]��。莫格利珠單抗是一款同類首 創(chuàng)的人源化單克隆抗體(mAb),靶向C-C趨化因子受體4(CCR4)[3]��,后者是在SS和MF癌癥細(xì)胞上存在持續(xù)表達(dá)的一種蛋白質(zhì)[4],[5],[6]�����。一旦惠爾金®與CCR4相結(jié)合�,會(huì)在人體免疫系統(tǒng)中激活更多的免疫細(xì)胞,進(jìn)而破壞癌細(xì)胞[7]��。
皮膚T細(xì)胞淋巴瘤(CTCL)屬于罕見型非霍奇金淋巴瘤�,SS和MF是CTCL的最常見的兩種亞型[8],可累及患者皮膚�、血液、淋巴結(jié)和內(nèi)臟器官[9]���。CTCL較罕見�����,每10萬人中約有24名患者[10]�。歐洲MF的年發(fā)病率約為1/11萬~1/35萬[11]�,而SS的年發(fā)病率為1/1000萬[12]。這兩種亞型加起來約占所有CTCL病例的65%[9]�����?�;颊咂毡樯钯|(zhì)量差���、誤診率高且晚期缺乏靶向治療藥物��,通常會(huì)出現(xiàn)皮損�、發(fā)癢�����、疼痛以及不可預(yù)知的皮膚癥狀��,并可能會(huì)導(dǎo)致進(jìn)一步的并發(fā)癥���,從而影響他們的預(yù)期壽命[3]��,[13]��。由于CTCL與濕疹及牛皮癬等常見皮膚病相似[14]�,患者平均需要2-7年才能得到確診[15]���。晚期患者的預(yù)后明顯更差�,約半數(shù)患者(52%)的生存期僅為5年[16]。
協(xié)和麒麟中國總經(jīng)理李韻表示:"惠爾金®于2021年7月獲得藥品審評(píng)中心授予的優(yōu)先審評(píng)資格�����,現(xiàn)已獲國家藥品監(jiān)督管理局的正式批準(zhǔn)�����。我們感謝監(jiān)管機(jī)構(gòu)對莫格利珠單抗的加速批準(zhǔn)��,這展示了政府為具有高度未被滿足醫(yī)療需求的中國患者帶來創(chuàng)新藥物的決心�����。這也為中國的塞扎里綜合征和蕈樣肉芽腫患者帶來了希望�����,他們將能獲得我們這款同類首 創(chuàng)藥物�����。協(xié)和麒麟通過追求生命科學(xué)和技術(shù)的進(jìn)步來創(chuàng)造新的價(jià)值��,我們致力于將更多創(chuàng)新性藥物帶入中國,從而造福廣大中國患者����。"
中國醫(yī)學(xué)科學(xué)院腫瘤醫(yī)院石遠(yuǎn)凱教授表示:"塞扎里綜合征和蕈樣肉芽腫給患者的生活質(zhì)量帶來了沉重的負(fù)擔(dān)����。莫格利珠單抗的獲批上市,將為中國這類患者帶來一種全新作用機(jī)制的治療選擇����。莫格利珠單抗改善了患者癥狀和生活質(zhì)量,患者的皮膚病變和血液學(xué)指標(biāo)對莫格利珠單抗治療呈現(xiàn)出顯著和持久的效果�����,中位無進(jìn)展生存期顯著延長���。"
此次獲批是基于MAVORIC研究的結(jié)果����。該研究是目前針對SS和MF患者最大規(guī)模的臨床試驗(yàn)[3]���。研究結(jié)果表明�,惠爾金®組患者的疾病控制時(shí)間是對照藥物伏立諾他組患者的兩倍多(中位無進(jìn)展生存期:7.7個(gè)月 vs 3.1個(gè)月)[3]。在處于各疾病階段的MF/SS患者中�����,惠爾金®的應(yīng)答率均高于伏立諾他*[3]�。惠爾金®和伏立諾他組患者的確認(rèn)總緩解率分別為28%和5%(p<0.001)[3]�����?;轄柦?reg;的總體耐受性良好,安全性可控[2]�����,[17]�。
MAVORIC研究還評(píng)估了患者報(bào)告的癥狀體驗(yàn)和生活質(zhì)量(QoL)。結(jié)果表明���,與接受伏立諾他治療的患者相比����,接受惠爾金®的患者在癥狀�����、情緒、功能和整體生活質(zhì)量方面均得到改善�����,體現(xiàn)在大部分功能和癥狀領(lǐng)域����?����?傮w而言��,這些研究結(jié)果表明���,與伏立諾他組相比��,惠爾金®組患者的疾病及癌癥特異性狀況相關(guān)生活質(zhì)量和總生活質(zhì)量均得到改善�����,同時(shí)生活質(zhì)量快速惡化的風(fēng)險(xiǎn)呈具有統(tǒng)計(jì)學(xué)意義的顯著降低[18]�。
關(guān)于惠爾金®(莫格利珠單抗)
惠爾金®是一款同類首 創(chuàng)人源化單克隆抗體(mAb),旨在與C-C趨化因子受體4(CCR4)相結(jié)合����。惠爾金®與CCR4結(jié)合后�����,會(huì)在人體免疫系統(tǒng)中激活更多的免疫細(xì)胞��,進(jìn)而破壞癌細(xì)胞[7]��?���;轄柦?reg;使用協(xié)和麒麟專有的POTELLIGENT®技術(shù),可增強(qiáng)人體對治療的自然免疫反應(yīng)��,從而提高對癌細(xì)胞的殺傷力�。FDA已授予惠爾金®突破性療法和孤兒藥認(rèn)定[19],[20]。此外����,惠爾金®還于2016年被歐盟委員會(huì)(EC)授予孤兒藥認(rèn)定[21]?;轄柦?reg;是首 個(gè)也是唯一在中國和世界其他地區(qū)獲批的靶向CCR4的生物制劑[22]��。
*伏立諾他是美國FDA批準(zhǔn)用于治療蕈樣肉芽腫和塞扎里綜合征的藥物�����,目前尚未在中國獲批
參考文獻(xiàn)
[1] Until July 2022, the data source: Ding Xiang Yuan database.
[2] Placeholder (To be updated with NMPA approval news release)
[3] Kim YH, Bagot M, Pinter-Brown L, et al. Mogamulizumab versus vorinostat in previously treated cutaneous T-cell lymphoma (MAVORIC): an international, open-label, randomised, controlled phase 3 trial. Lancet Oncol. 2018;19(9):1192-1204.
[4] Ferenczi K, Fuhlbrigge RC, Pinkus J, et al. Increased CCR4 expression in cutaneous T cell lymphoma. J Invest Dermatol. 2002;119:1405-10.
[5] Yoshie O, et al. Frequent Expression of CCR4 in Adult T-Cell Leukemia and Human T-cell Leukemia Virus Type 1-transformed T cells. Blood. 2002;99(5):1505-11.
[6] Ishida T, et al. Clinical Significance of CCR4 Expression in Adult T-cell Leukemia/Lymphoma: Its Close Association With Skin Involvement and Unfavorable Outcome. Clin Cancer Res. 2003;9:3625-34.
[7] Duvic M, et al. Mogamulizumab for the treatment of cutaneous T-cell lymphoma: recent advances and clinical potential. Ther Adv Hematol. 2016;7(3):171-174.
[8] Willemze R, et al. The 2018 update of the WHO-EORTC classification for primary cutaneous lymphomas. Blood. 2019;133(16):1703-1714.
[9] Olsen E, Vonderheid E, Pimpinelli N, et al. Revisions to the staging and classification of mycosis fungoides and Sezary syndrome: a proposal of the International Society for Cutaneous Lymphomas (ISCL) and the cutaneous lymphoma task force of the European Organization of Research and Treatment of Cancer (EORTC). Blood. 2007;110(6):1713-22.
[10] Orphanet: Prevalence and incidence of rare diseases: Bibliographic data. Available from: https://www.orpha.net/orphacom/cahiers/docs/GB/Prevalence_of_rare_diseases_by_decreasing_prevalence_or_cases.pdf. Last accessed: June 2020.
[11] Orphanet: Mycosis Fungoides. Available from: https://www.orpha.net/consor/cgi-bin/OC_Exp.php?Lng=GB&Expert=2584. Last Accessed: June 2020.
[12] Orphanet: Sézary syndrome. Available from: https://www.orpha.net/consor/cgi-bin/OC_Exp.php?Expert=3162. Last Accessed: June 2020.
[13] Haun P, et al. Fast Facts : Diagnosing Cutaneous T-Cell Lymphoma. Karger Publishing. 2016.
[14] Cutaneous Lymphoma Foundation, Lymphoma Action and Lymphoma Coalition Europe. Cutaneous lymphoma – a patient's guide. 2019. Available from: https://lymphoma-action.org.uk/sites/default/files/media/documents/2019-06/Cutaneous%20lymphoma%20-%20patient%26%23039%3Bs%20guide%20-%20English%20language%20source%20document%20-%20final%20version%20for%20publication%20-%20April%202019.pdf. Last accessed: June 2020.
[15] CL Foundation: A Patient's Guide. Available from: https://www.clfoundation.org/sites/default/files/2018-04/a_patients_guide.pdf. Last Accessed: 18 November 2019.
[16] Scarisbrick JJ, Prince M, Vermeer MH, et al. Cutaneous Lymphoma International Consortium Study of Outcome in Advanced Stages of Mycosis Fungoides and Sézary Syndrome: Effect of Specific Prognostic Markers on Survival and Development of a Prognostic Model. J Clin Oncol. 2015;33(32):3766-3773.
[17] Kim YH, Bagot M, Zinzani PL et al. Safety of Mogamulizumab in Mycosis Fungoides and Sézary Syndrome: Final Results from the Phase 3 Mavoric Study. Blood. 2019;134 (1):5300.
[18] Clin Lymphoma Myeloma Leuk. 2021 Feb; 21(2):97-105
[19] Search Orphan Drug Designations and Approvals (fda.gov). Available from https://www.accessdata.fda.gov/scripts/opdlisting/oopd/detailedIndex.cfm?cfgridkey=322010. Last accessed: July 2022.
[20] FDA approves treatment for two rare types of non-Hodgkin lymphoma. Available from: https://www.fda.gov/news-events/press-announcements/fda-approves-treatment-two-rare-types-non-hodgkin-lymphoma. Last accessed: July 2022.
[21] EU/3/16/1756: Orphan designation for the treatment of cutaneous T-cell lymphoma. Available from: https://www.ema.europa.eu/en/medicines/human/orphan-designations/eu3161756. Last accessed: July 2022.
