Barros Melca M O, Yamamoto Mihoko, Figueiredo Maria S, Cançado Rodolfo, Kimura Elisa Y S, Langhi Dante M, Chiattone Carlos S, Bordin Jose O
Faculdade de Ciências Médicas, Universidade Federal de São Paulo, Santa Casa de São Paulo, São Paulo, Brasil.
Transfusion. 2009 Jan;49(1):154-60. doi: 10.1111/j.1537-2995.2008.01936.x. Epub 2008 Oct 2.
Animal models have shown that CD47-deficient mice develop severe autoimmune hemolytic anemia (AIHA) because the binding of red blood cell (RBC) CD47 to signal-regulatory protein (SIRP-alpha) on macrophages contributes to the inhibition of phagocytosis. In contrast, complement-inhibitory proteins such as CD35, CD55, and CD59 may protect RBCs against the lysis by complement.
With the use of flow cytometric analyses, the expression of CD47, CD35, CD55, and CD59 on RBCs and of SIRP-alpha,beta on peripheral monocytes of 36 patients with warm AIHA (wAIHA; 23 with active wAIHA, 13 with wAIHA in remission) and 20 healthy subjects was evaluated.
The mean fluorescence intensities (MFIs) of the expression of CD47, CD35, CD55, and SIRP-alpha,beta of active wAIHA patients, wAIHA in remission, and healthy subjects were not statistically different. Patients with active wAIHA showed significantly lower CD59 expression on RBCs than healthy individuals (MFI, 512.5 +/- 59.6 vs. 553.7 +/- 36.6; p = 0.009), while the CD59 expression in patients with wAIHA in remission was not significantly different from that of healthy controls (MFI, 538.4 +/- 48.3 vs. 553.7 +/- 36.6; p > 0.05). The expression of CD59 on RBCs of 3 patients who died from the wAIHA was lower than that seen on RBCs of healthy controls (MFI, 433.6 +/- 69.6 vs. 553.74 +/- 36.6; p = 0.0001).
Our data show that the expression of CD47 on RBCs and SIRP-alpha,beta on monocytes of patients with wAIHA is not different from that seen in healthy individuals. In addition, we detected that patients with active wAIHA present low expression of CD59 and normal expression of CD35 and CD55 on their RBCs. Complement-regulatory proteins may play an important role in protecting RBC destruction through the activation of complement.
动物模型表明,CD47缺陷小鼠会发生严重的自身免疫性溶血性贫血(AIHA),因为红细胞(RBC)上的CD47与巨噬细胞上的信号调节蛋白(SIRP-α)结合有助于抑制吞噬作用。相比之下,补体抑制蛋白如CD35、CD55和CD59可保护红细胞免受补体介导的裂解。
通过流式细胞术分析,评估了36例温抗体型自身免疫性溶血性贫血(wAIHA;23例活动期wAIHA,13例缓解期wAIHA)患者红细胞上CD47、CD35、CD55和CD59以及外周血单核细胞上SIRP-α、β的表达,并与20名健康受试者进行比较。
活动期wAIHA患者、缓解期wAIHA患者和健康受试者的CD47、CD35、CD55以及SIRP-α、β表达的平均荧光强度(MFI)无统计学差异。活动期wAIHA患者红细胞上的CD59表达显著低于健康个体(MFI:512.5±59.6 vs. 553.7±36.6;p = 0.009),而缓解期wAIHA患者的CD59表达与健康对照无显著差异(MFI:538.4±48.3 vs. 553.7±36.6;p>0.05)。3例死于wAIHA患者的红细胞上CD59表达低于健康对照(MFI:433.6±69.6 vs. 553.74±36.6;p = 0.0001)。
我们的数据表明,wAIHA患者红细胞上CD47以及单核细胞上SIRP-α、β的表达与健康个体无异。此外,我们检测到活动期wAIHA患者红细胞上CD59表达降低,而CD35和CD55表达正常。补体调节蛋白可能在通过补体激活保护红细胞免受破坏中起重要作用。
