利妥昔单抗阻碍慢性疲劳综合征/肌痛性脑脊髓炎患者的自然杀伤细胞功能:一项体外初步研究。
Rituximab impedes natural killer cell function in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis patients: A pilot in vitro investigation.
作者信息
Eaton Natalie, Cabanas Hélène, Balinas Cassandra, Klein Anne, Staines Donald, Marshall-Gradisnik Sonya
机构信息
School of Medical Science, Griffith University, QLD, Gold Coast, Australia.
The National Centre for Neuroimmunology and Emerging Diseases, Menzies Health Institute Queensland, Griffith University, QLD, Gold Coast, Australia.
出版信息
BMC Pharmacol Toxicol. 2018 Mar 27;19(1):12. doi: 10.1186/s40360-018-0203-8.
BACKGROUND
A recent in vitro pilot investigation reported Rituximab significantly reduced natural killer (NK) cell cytotoxicity in healthy donors. Chronic fatigue syndrome/Myalgic encephalomyelitis (CFS/ME) is a debilitating disorder of unknown etiology. A consistent finding is a significant reduction in NK cell cytotoxicity. Rituximab has been reported having questionable potential therapeutic benefits for the treatment of CFS/ME, however, the potential effects of Rituximab on NK cell cytotoxicity in CFS/ME patients are yet to be determined.
METHODS
A total of eight CFS/ME patients (48.63 ± 15.69 years) and nine non-fatigued controls (NFC) (37.56 ± 11.06 years) were included using the Fukuda case definition. Apoptotic function, lytic proteins and degranulation markers were measured on isolated NK cells using flow cytometry following overnight incubation with Rituximab at 10 μg/ml and 100 μg/ml.
RESULTS
There was a significant reduction in NK cell lysis between CFS/ME patients and NFC following incubation with Rituximab at 100 μg/ml at 12.5:1 and 6.25:1 effecter-target (E:T) ratios (p < 0.05). However, there was no significant difference for NFC following incubation with Rituximab at 10 μg/ml and 100 μg/ml. There was no significant difference between CFS/ME patients and NFC for granzyme A and granzyme B prior to incubation with Rituximab and following overnight incubation with Rituximab at 10 μg/ml. There was a significant decrease in granzyme B in CFS/ME patients compared to NFC with 100 μg/ml of Rituximab prior to K562 cells stimulation (p < 0.05). There was a significant increase in CD107a (p < 0.05) and CD107b expression (p < 0.01) in NFC after stimulation with K562 cells prior to incubation with Rituximab. There was a significant increase in CD107b expression between CFS/ME patients and NFC prior to incubation with Rituximab and without stimulation of K562 cells (p < 0.01). Importantly, there was a significant increase in CD107b following overnight incubation with 100 μg/ml of Rituximab in NFC prior to K562 cells stimulation (p < 0.01).
CONCLUSION
This study reports significant decreases in NK cell lysis and a significant increase in NK cell degranulation following Rituximab incubation in vitro in CFS/ME patients, suggesting Rituximab may be toxic for NK cells. Caution should be observed in clinical trials until further investigations in a safe and controlled in vitro setting are completed.
背景
最近一项体外初步研究报告称,利妥昔单抗可显著降低健康供体中自然杀伤(NK)细胞的细胞毒性。慢性疲劳综合征/肌痛性脑脊髓炎(CFS/ME)是一种病因不明的使人衰弱的疾病。一个一致的发现是NK细胞细胞毒性显著降低。据报道,利妥昔单抗对CFS/ME的治疗具有潜在的治疗益处,但利妥昔单抗对CFS/ME患者NK细胞细胞毒性的潜在影响尚未确定。
方法
采用福田病例定义,纳入了8例CFS/ME患者(48.63±15.69岁)和9例非疲劳对照(NFC)(37.56±11.06岁)。在与10μg/ml和100μg/ml的利妥昔单抗过夜孵育后,使用流式细胞术测量分离的NK细胞上的凋亡功能、溶解蛋白和脱颗粒标记物。
结果
在效应细胞与靶细胞(E:T)比例为12.5:1和6.25:1时,100μg/ml利妥昔单抗孵育后,CFS/ME患者与NFC之间的NK细胞裂解显著降低(p<0.05)。然而,10μg/ml和100μg/ml利妥昔单抗孵育后,NFC之间无显著差异。在与利妥昔单抗孵育前以及与10μg/ml利妥昔单抗过夜孵育后,CFS/ME患者与NFC之间的颗粒酶A和颗粒酶B无显著差异。在K562细胞刺激前,与100μg/ml利妥昔单抗孵育的CFS/ME患者与NFC相比,颗粒酶B显著降低(p<0.05)。在与利妥昔单抗孵育前,用K562细胞刺激后,NFC中CD107a(p<0.05)和CD107b表达显著增加(p<0.01)。在与利妥昔单抗孵育前且未刺激K562细胞的情况下,CFS/ME患者与NFC之间的CD107b表达显著增加(p<0.01)。重要的是,在K562细胞刺激前,NFC中与100μg/ml利妥昔单抗过夜孵育后,CD107b显著增加(p<0.01)。
结论
本研究报告称,体外利妥昔单抗孵育后,CFS/ME患者的NK细胞裂解显著降低,NK细胞脱颗粒显著增加,提示利妥昔单抗可能对NK细胞有毒性。在安全可控的体外环境中完成进一步研究之前,临床试验中应谨慎观察。
Zotero 插件