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北京大学学报(医学版) ›› 2019, Vol. 51 ›› Issue (3): 591-595. doi: 10.19723/j.issn.1671-167X.2019.03.032

• 技术方法 • 上一篇    下一篇

原发性肝癌患者同种异体NK细胞治疗后疗效评价及外周淋巴细胞亚群变化特点

谢云波,张纪元,杜美玲,孟繁平,福军亮,刘利敏,王松山,曲芮,廉方,乔菲,陈杨柳,高莹莹,徐若男,施明,王福生()   

  1. 解放军总医院第五医学中心感染性疾病诊疗与研究中心, 北京 100039
  • 收稿日期:2019-03-18 出版日期:2019-05-09 发布日期:2019-06-26
  • 作者简介:王福生,中国科学院院士,教授,主任医师,博士生导师。国家杰出青年基金获得者,国家自然科学基金创新研究群体牵头人,国家感染性疾病临床医学研究中心牵头人,解放军总医院第五医学中心感染病诊疗与研究中心主任。擅长病毒性肝炎、艾滋病和疑难危重肝病的临床诊治工作,并结合临床难题开展研究,系统地揭示了乙型肝炎临床免疫学特征及肝脏损伤机制,提出了优化慢性乙肝抗病毒治疗与免疫应答恢复的“爬坡假说”,阐明了艾滋病免疫重建失败的关键机制,开拓了疑难肝病和艾滋病细胞治疗与研究的新方向。曾先后主持多项国家重大科研项目,以通信作者在N Engl J MedGastroenterologyHepatologyBlood等期刊发表论文160余篇,获得国家科技进步奖二等奖3项、省部级奖一等奖3项。
  • 基金资助:
    国家自然科学基金(81721002,81571567)

Efficacy and peripheral immunity analysis of allogeneic natural killer cells therapy in patients with hepatocellular carcinoma

Yun-bo XIE,Ji-yuan ZHANG,Mei-ling DU,Fan-ping MENG,Jun-liang FU,Li-min LIU,Song-shan WANG,Rui QU,Fang LIAN,Fei QIAO,Yang-liu CHEN,Ying-ying GAO,Ruo-nan XU,Ming SHI,Fu-sheng WANG()   

  1. Institute of Infectious Diseases, the Fifth Medical Center of PLA General Hospital, Beijing 100039, China
  • Received:2019-03-18 Online:2019-05-09 Published:2019-06-26
  • Supported by:
    Supported by the National Natural Science Foundation of China(81721002,81571567)

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摘要: 目的 评估同种异体自然杀伤(natural killer, NK)细胞治疗原发性肝癌的安全性和有效性,并探讨其抗肿瘤机制。方法 对21例经同种异体NK细胞治疗的原发性肝细胞癌患者进行1年随访,通过对其生存期、影像学指标、血液学指标、生物化学指标及免疫学指标分析,评价该治疗的安全性和有效性,分析患者经过治疗后外周血淋巴细胞亚群的变化。结果 (1)21例原发性肝癌患者中,11例患者治疗1次,5例患者治疗2次,5例患者治疗3次,患者治疗后未见严重不良反应,10例患者有一过性发热,1例患者出现肝区疼痛,1例患者出现头痛,未经治疗均于8 h内自行缓解;(2)在一年随访中,总疾病控制率为76.2%,其中Barcelona分期(Barcelona clinic liver cancer, BCLC)A期患者中疾病控制率为100%, 病情稳定(stable disease, SD)10例;BCLC B期患者中疾病控制率为60%,部分缓解(partial response, PR)1例,SD 2例;BCLC C期患者中疾病控制率为50%,完全缓解(complete response, CR)1例,PR 2例;(3)患者治疗后24 h外周血NK细胞和CD8+T细胞频率较治疗前显著降低,CD4+T细胞频率和CD4/CD8较治疗前显著上升。结论 同种异体NK细胞治疗原发性肝细胞癌有很好的安全性和有效性。

关键词: NK细胞, 肝细胞癌, 同种异体, 外周免疫

Abstract: Objective: To evaluate the safety and efficacy of allogeneic natural killer (NK) cells in the treatment of primary hepatocellular carcinoma (HCC), and to elucidate the mechanism of NK cells therapy.Methods: Twenty-one patients with primary HCC treated with allogeneic NK cells at the Fifth Medical Center of the PLA General Hospital were followed up for 1 year. Peripheral blood mononuclear cells (PBMCs) were isolated from patient-related donors and cultured in vitro for 15 days and infused to the patients in two consecutive days. Clinical data and laboratory data were collected and analyzed, including survival, clinical features, imaging changes, hematology, immunology, and biochemical indicators to evaluate the safety and efficacy of allogeneic NK cell therapy. The changes of peripheral blood lymphocyte subsets after treatment were also analyzed to explore the possible anti-tumor mechanisms. Results: (1) Of the 21 patients with primary HCC, 11 patients were treated once, 5 patients were treated twice, and 5 patients were treated 3 times. After allogeneic NK cells infusion, 10 patients had fever, 1 patient had slight hepatalgia and 1 patient had slight headache, no other adverse events occurred including acute and chronic graft-versus-host disease (GVHD). They resolved spontaneously within 8 hours without other treatment. (2) The total disease control rate was 76.2% during one-year follow-up. Among them, the patients with Barcelona clinic liver cancer (BCLC) stage A had a disease control rate of 100%, stable disease (SD) in 10 cases; BCLC stage B patients had a disease control rate of 60%, partial response (PR) in 1 case, and SD 2 in cases; BCLC stage C patients had a disease control rate of 50%, complete response (CR) in 1 case, and 2 cases of PR. (3) The frequencies of NK cells and CD8+ T cells in peripheral blood were significantly lower than that before at 24 hours after treatment, and the frequencies of CD4+ T cells and CD4/CD8 were significantly higher than the baseline.Conclusion: Allogeneic NK cells have good safety and efficacy in the treatment of primary HCC. The anti-tumor effect of the allogeneic NK cells may play an important role in the activation of the patient’s natural immune system and delay disease progression, suggesting that allogeneic NK cells combined with sorafenib may be a very effective treatment for advanced HCC, and further large-sample multicenter randomized controlled clinical trials are needed to validate this result.

Key words: Natural killer cells, Hepatocellular carcinoma, Allogeneic, Lymphocyte subsets

中图分类号: 

  • R735.7

表1

患者的人口学和基线特征"

Variable Data
Age/years 56.1±7.6
Gender, n(%)
Male 18 (86)
Female 3 (14)
Cause ofdisease, n(%)
Alcoholic liver disease 1 (5)
Hepatitis B only 16 (76)
Other 4 (19)
ECOG performancestatus, n(%)
0 8 (38)
1 11 (52)
2 2 (10)
BCLC stage, n(%)
A 10 (48)
B 5 (24)
C 6 (28)
Child-Pugh class, n(%)
A 17(81)
B 4(19)
Biochemical analysis
albumin/(g/L)
Median 40.6
Range 27.0-46.0
Totalbilirubin/(μmol/L)
Median 14.3
Range 8.9-63.6
Alpha-fetoprotein/(μg/L)
Median 20.6
Range 2.2-1210.0

表2

NK细胞治疗疗效评价"

BCLC staging Total Complete response (CR) Partialresponse (PR) Stable disease (SD) Disease-control rate/%
A 10 0 0 10 (100%) 100
B 5 0 1 (20%) 2 (40%) 60
C 6 1 (17%) 2 (33%) 0 50

图1

NK细胞治疗24 h后患者外周血淋巴细胞亚群变化"

[1] Boni C, Lampertico P, Talamona L , et al. Natural killer cell phenotype modulation and natural killer/T-cell interplay in nucleos(t)ide analogue-treated hepatitis e antigen-negative patients with chronic hepatitis B[J]. Hepatology, 2015,62(6):1697-1709.
doi: 10.1002/hep.28155
[2] Cai L, Zhang Z, Zhou L , et al. Functional impairment in circulating and intrahepatic NK cells and relative mechanism in hepatocellular carcinoma patients[J]. Clin Immunol, 2008,129(3):428-437.
doi: 10.1016/j.clim.2008.08.012
[3] Easom NJW, Stegmann KA, Swadling L , et al. IL-15 overcomes hepatocellular carcinoma-induced NK cell dysfunction[J]. Front Immunol, 2018,9:1009.
doi: 10.3389/fimmu.2018.01009
[4] Liu P, Chen L, Zhang H. Natural killer cells in liver disease and hepatocellular carcinoma and the NK cell-based immunotherapy [J/OL]. J Immunol Res, 2018, 2018: 1206737.( 2018-09-04)[2019-03-01].https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6142725/ .
[5] Parkhurst MR, Riley JP, Dudley ME , et al. Adoptive transfer of autologous natural killer cells leads to high levels of circulating natural killer cells but does not mediate tumor regression[J]. Clin Cancer Res, 2011,17(19):6287-6297.
doi: 10.1158/1078-0432.CCR-11-1347
[6] Guillerey C, Huntington ND, Smyth MJ . Targeting natural killer cells in cancer immunotherapy[J]. Nat Immunol, 2016,17(9):1025-1036.
doi: 10.1038/ni.3518
[7] Eisenhauer EA, Therasse P, Bogaerts J , et al. New response evaluation criteria in solid tumours: revised RECIST guideline (version 1.1)[J]. Eur J Cancer, 2009,45(2):228-247.
doi: 10.1016/j.ejca.2008.10.026
[8] Wong PPC, Kariminia A, Jones D , et al. Plerixafor effectively mobilizes CD56 (bright) NK cells in blood, providing an allograft predicted to protect against GVHD[J]. Blood, 2018,131(25):2863-2866.
doi: 10.1182/blood-2018-03-836700
[9] Ullrich E, Salzmann-Manrique E, Bakhtiar S , et al. Relation between acute GVHD and NK cell subset reconstitution following allogeneic stem cell transplantation[J]. Front Immunol, 2016,7:595.
[10] Kariminia A, Ivison S, Ng B , et al. CD56 (bright) natural killer regulatory cells in filgrastim primed donor blood or marrow products regulate chronic graft-versus-host disease: the Canadian Blood and Marrow Transplant Group randomized 0601 study results[J]. Haematologica, 2017,102(11):1936-1946.
doi: 10.3324/haematol.2017.170928
[11] Qin Z, Chen J, Zeng J , et al. Effect of NK cell immunotherapy on immune function in patients with hepatic carcinoma: a preliminary clinical study[J]. Cancer Biol Ther, 2017,18(5):323-330.
doi: 10.1080/15384047.2017.1310346
[12] Miller JS, Soignier Y, Panoskaltsis-Mortari A , et al. Successful adoptive transfer and in vivo expansion of human haploidentical NK cells in patients with cancer[J]. Blood, 2005,105(8):3051-3057.
doi: 10.1182/blood-2004-07-2974
[13] Llovet JM, Ricci S, Mazzaferro V , et al. Sorafenib in advanced hepatocellular carcinoma[J]. N Engl J Med, 2008,359(4):378-390.
doi: 10.1056/NEJMoa0708857
[14] Kohga K, Takehara T, Tatsumi T , et al. Sorafenib inhibits the shedding of major histocompatibility complex class Ⅰ-related chain A on hepatocellular carcinoma cells by down-regulating a disintegrin and metalloproteinase 9[J]. Hepatology, 2010,51(4):1264-1273.
doi: 10.1002/hep.23456
[15] Sprinzl MF, Reisinger F, Puschnik A , et al. Sorafenib perpetuates cellular anticancer effector functions by modulating the crosstalk between macrophages and natural killer cells[J]. Hepatology, 2013,57(6):2358-2368.
doi: 10.1002/hep.26328
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ISSN 1671-167X
CN 11-4691/R
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