Simon Toby L, FitzGerald Peter, Kühne Mirjam, Farrar Connie, Knowles Jonathan, Bycholski Keith, Zenker Othmar
CSL Plasma, Boca Raton, Florida.
CSL Plasma Laboratory, Knoxville, Tennessee.
Transfusion. 2018 Dec;58 Suppl 3:3065-3071. doi: 10.1111/trf.15014.
To ensure that immunoglobulin (Ig) products have adequate functional antibody, the US Food and Drug Administration (FDA) requires that Ig lots contain minimum levels of measles neutralizing antibody; the current minimum is 0.48 x US Reference Ig 176.
In the first part of the study, measles antibody titers were measured in donor plasma samples collected in 2007, 2011, and 2017. In the second part, trough or steady-state serum levels of measles neutralizing antibody were measured in two studies of patients with primary immunodeficiency (PID) who were treated with intravenous (Study 1; N = 46) or subcutaneous (Study 2; N = 18) Ig replacement therapy, meeting previous requirements for lot potency (≥0.6 x US Reference Ig 176). Serum measles neutralizing antibody titers were then estimated for conditions in which the potency of the Ig replacement product was 0.48 or 0.30 x US Reference Ig 176.
Measles antibody titers in donated plasma samples declined in donors born after 1963. In the two studies of patients with PID who were treated with intravenous or subcutaneous Ig replacement therapy, all patients exhibited trough (intravenous Ig) or steady-state (subcutaneous Ig) measles neutralizing antibody titers above 0.12 IU/mL, which has been shown to protect against clinical measles in the general population. Estimates suggest that all patients except one would have continued to meet this standard if the Ig lot potency had been 0.48 or 0.30 x US Reference Ig 176.
These studies provide supporting evidence that the lot release specification can be safely lowered from 0.48 to 0.30 x US Reference Ig 176, which will accommodate declining measles neutralizing antibody levels in donor plasma.
为确保免疫球蛋白(Ig)产品具有足够的功能性抗体,美国食品药品监督管理局(FDA)要求Ig批次含有最低水平的麻疹中和抗体;目前的最低水平是0.48×美国参考Ig 176。
在研究的第一部分,对2007年、2011年和2017年采集的供体血浆样本中的麻疹抗体滴度进行了测量。在第二部分中,在两项针对原发性免疫缺陷(PID)患者的研究中,测量了接受静脉注射(研究1;N = 46)或皮下注射(研究2;N = 18)Ig替代疗法的患者的麻疹中和抗体谷值或稳态血清水平,这些患者的治疗符合先前的批次效力要求(≥0.6×美国参考Ig 176)。然后估计了Ig替代产品效力为0.48或0.30×美国参考Ig 176时的血清麻疹中和抗体滴度情况。
1963年后出生的供体所捐献血浆样本中的麻疹抗体滴度下降。在两项针对接受静脉或皮下Ig替代疗法的PID患者的研究中,所有患者的麻疹中和抗体谷值(静脉注射Ig)或稳态(皮下注射Ig)滴度均高于0.12 IU/mL,这已被证明可在普通人群中预防临床麻疹。估计表明,如果Ig批次效力为0.48或0.30×美国参考Ig 176,除一名患者外,所有患者仍将继续符合该标准。
这些研究提供了支持性证据,表明批次放行规格可安全地从0.48×美国参考Ig 176降至0.30×美国参考Ig 176,这将适应供体血浆中麻疹中和抗体水平的下降。
