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人源Rh D单克隆抗体(BRAD - 3和BRAD - 5)可使Rh D+红细胞的清除加速,并抑制Rh D阴性志愿者的Rh D免疫反应。

Human Rh D monoclonal antibodies (BRAD-3 and BRAD-5) cause accelerated clearance of Rh D+ red blood cells and suppression of Rh D immunization in Rh D- volunteers.

作者信息

Kumpel B M, Goodrick M J, Pamphilon D H, Fraser I D, Poole G D, Morse C, Standen G R, Chapman G E, Thomas D P, Anstee D J

机构信息

International Blood Group Reference Laboratory, Bristol, UK.

出版信息

Blood. 1995 Sep 1;86(5):1701-9.

PMID:7655002
Abstract

The use of prophylactic anti-D to prevent Rh D immunization in Rh D- women and subsequent hemolytic disease in Rh D+ infants is widespread, but has led to shortages of the anti-D Ig. With the aim of substituting monoclonal anti-D for Rh D prophylaxis, we have compared the abilities of monoclonal and polyclonal anti-D to clear Rh D+ red blood cells (RBCs) infused into Rh D- male volunteers and to suppress Rh D immunization. Two human monoclonal antibodies (MoAbs), BRAD-3 (IgG3) and BRAD-5 (IgG1), produced from stable Epstein-Barr virus-transformed B-lymphoblastoid cell lines, were selected because of their proven in vitro activity in promoting RBC lysis in antibody-dependent cell-mediated cytotoxicity assays. RBC clearance was assessed by intravenous injection of 3 mL of 51chromium-labeled D+ RBCs into 27 volunteers 48 hours after intramuscular injection of monoclonal or polyclonal anti-D. Further 3-mL injections of unlabeled D+ cells were administered at 6 and 9 months to induce immunization. Blood samples were taken throughout the 12-month period of study for the serologic detection of anti-D. The mean half-life (t50%) of RBCs in 7 recipients of 300 micrograms BRAD-5 (5.9 hours) was similar to that in 8 recipients of 500 IU polyclonal anti-D (5.0 hours), whereas D+ cells were cleared more slowly in some of the 8 subjects injected with 300 micrograms BRAD-3 (mean t50% 12.7 hours) and in 1 individual administered 100 micrograms BRAD-3 (t50% 41.0 hours). The rate of RBC clearance in both groups administered 300 micrograms monoclonal anti-D correlated with the amount of antibody bound per cell, determined by flow cytometry. There was no evidence of primary immunization having occurred in any subject after 6 months of follow-up. Five of 24 subjects produced anti-D after one or two further injections of RBCs, confirming that they were responders who had been protected by the monoclonal or polyclonal anti-D administered initially. Four of these responders were recipients of monoclonal anti-D (3 BRAD-3, 1 BRAD-5). One individual who received BRAD-5 produced accelerated clearance of D+ RBCs at the third unprotected RBC challenge but did not seroconvert. This study shows that the human MoAbs BRAD-3 and BRAD-5 can prevent Rh D immunization, and indicates that they may be suitable replacements for the polyclonal anti-D presently used in prophylaxis of Rh D hemolytic disease of the newborn.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在Rh D阴性女性中使用预防性抗-D以预防Rh D免疫,并预防Rh D阳性婴儿随后发生溶血病的做法很普遍,但这导致了抗-D免疫球蛋白的短缺。为了用单克隆抗-D替代Rh D预防措施,我们比较了单克隆和多克隆抗-D清除注入Rh D阴性男性志愿者体内的Rh D阳性红细胞(RBC)以及抑制Rh D免疫的能力。选择了两种由稳定的爱泼斯坦-巴尔病毒转化的B淋巴细胞系产生的人单克隆抗体(MoAbs),即BRAD-3(IgG3)和BRAD-5(IgG1),因为它们在抗体依赖性细胞介导的细胞毒性试验中具有促进RBC裂解的体外活性。在肌肉注射单克隆或多克隆抗-D 48小时后,通过向27名志愿者静脉注射3 mL 51铬标记的D+ RBC来评估RBC清除情况。在6个月和9个月时再注射3 mL未标记的D+细胞以诱导免疫。在整个12个月的研究期间采集血样用于抗-D的血清学检测。7名接受300微克BRAD-5的受试者中RBC的平均半衰期(t50%)为5.9小时,与8名接受500 IU多克隆抗-D的受试者(5.0小时)相似,而在8名注射300微克BRAD-3的受试者中的一些以及1名接受100微克BRAD-3的受试者(t50%为41.0小时)中,D+细胞清除得更慢。两组接受300微克单克隆抗-D的RBC清除率与通过流式细胞术测定的每个细胞结合的抗体量相关。随访6个月后,没有证据表明任何受试者发生了初次免疫。24名受试者中有5名在再注射一两次RBC后产生了抗-D,证实他们是反应者,最初接受的单克隆或多克隆抗-D对其起到了保护作用。这些反应者中有4名是单克隆抗-D的接受者(3名BRAD-3,1名BRAD-5)。一名接受BRAD-5的个体在第三次未受保护的RBC攻击时D+ RBC清除加速,但未发生血清转化。这项研究表明,人MoAbs BRAD-3和BRAD-5可以预防Rh D免疫,并表明它们可能是目前用于预防新生儿Rh D溶血病的多克隆抗-D的合适替代品。(摘要截短至400字)

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