骨髓移植后输血后紫癜

Evenson D A, Stroncek D F, Pulkrabek S, Perry E H, Radford J, Miller J S, Verfaillie C

Department of Laboratory Medicine and Pathology, University of Minnesota Hospitals and Clinics, St. Paul, Minnesota, USA.

Transfusion. 1995 Aug;35(8):688-93. doi: 10.1046/j.1537-2995.1995.35895357902.x.

BACKGROUND

Thrombocytopenia is a major cause of morbidity and hospital expense following bone marrow transplantation. Platelet transfusions in these patients are frequently complicated by the recipient's development of antibodies to HLA class I antigens. When these patients become refractory to the transfusion of HLA-matched platelets, the recipient's platelet antigen phenotype must be determined, to ensure that donor platelets will be phenotypically compatible. Cases of alloimmunization to HPA-1a and HPA-1b resulting in refractoriness to transfused platelets and the subsequent development of a posttransfusion purpura-like syndrome are reported.

CASE REPORTS

In the first case, a 43-year-old woman with Stage IV infiltrating ductal breast cancer presented to the hospital for a transplant of autologous peripheral blood stem cells. After the transplant, her platelet count remained less than 10 x 10(9) per L, despite daily platelet transfusions, including HLA-matched platelets. Fourteen days following the transplant, her serum was found to contain anti-HPA-1a. Initially, the patient was refractory to the transfusion of HPA-1a-negative platelets, but after treatment with intravenous immunoglobulin, she had transient increases in posttransfusion platelet counts. She was also treated with a staphylococcal protein A immunoadsorption column and has not had any such subsequent refractoriness. Her genotype has been found, by use of allele-specific oligonucleotide hybridization with white cell DNA, to be HPA-1b/1b. The second case involved a 32-year-old woman with chronic myelogenous leukemia who received an unrelated-donor marrow transplant. Three years later, her CML recurred, and she was treated with interferon-alpha. Four months afterward, she experienced interferon-alpha-induced thrombocytopenia and the interferon therapy was discontinued. She received 12 platelet transfusions in 20 days, but none was effective. Antibodies specific for HLA antigens and HPA-1b were detected, and three HLA-matched, HPA-1b-negative apheresis platelet components were given, but without effect. Two days after treatment with methylprednisolone (1 g intravenously) and prednisone (2 mg/kg/day orally), her platelet count was 26 x 10(9) per L, and after 8 more days, it was 102 x 10(9) per L, without further transfusions. She was found to be homozygous for HPA-1a (HPA-1a/1a).

CONCLUSION

Anti-HPA-1a and anti-HPA-1b can cause refractoriness to platelet transfusions in bone marrow transplant patients. Testing for platelet-specific antibodies should be considered in all patients who are refractory to HLA-matched platelets.

背景

血小板减少是骨髓移植后发病和住院费用的主要原因。这些患者的血小板输注常常因受者产生针对HLA I类抗原的抗体而变得复杂。当这些患者对输注HLA匹配的血小板产生耐受时，必须确定受者的血小板抗原表型，以确保供体血小板在表型上是相容的。有报道称，对HPA-1a和HPA-1b发生同种免疫反应，导致对输注血小板产生耐受，并随后出现类似输血后紫癜的综合征。

病例报告

在第一个病例中，一名43岁患有IV期浸润性导管乳腺癌的女性因自体外周血干细胞移植入院。移植后，尽管每日输注血小板，包括HLA匹配的血小板，她的血小板计数仍低于10×10⁹/L。移植后14天，发现她的血清中含有抗HPA-1a。最初，患者对输注HPA-1a阴性血小板产生耐受，但在接受静脉注射免疫球蛋白治疗后，她输血后的血小板计数出现短暂升高。她还接受了葡萄球菌蛋白A免疫吸附柱治疗，此后未再出现此类耐受情况。通过使用等位基因特异性寡核苷酸与白细胞DNA杂交，发现她的基因型为HPA-1b/1b。第二个病例涉及一名32岁患有慢性粒细胞白血病的女性，她接受了无关供体骨髓移植。三年后，她的慢性粒细胞白血病复发，接受了α干扰素治疗。四个月后，她出现了α干扰素诱导的血小板减少，于是停止了干扰素治疗。她在20天内接受了12次血小板输注，但均无效。检测到针对HLA抗原和HPA-1b的特异性抗体，给予了3个HLA匹配、HPA-1b阴性的单采血小板成分，但无效。在静脉注射甲泼尼龙（1g）和口服泼尼松（2mg/kg/天）治疗两天后，她的血小板计数为26×10⁹/L，再过8天后，血小板计数为102×10⁹/L，无需进一步输血。发现她为HPA-1a纯合子（HPA-1a/1a）。