2657例非肿瘤性疾病住院患者红细胞外非自身免疫性获得性溶血性贫血病因分析

Q3 Medicine Clinical Medicine Insights- Pathology Pub Date : 2014-04-15 eCollection Date: 2014-01-01 DOI:10.4137/CPath.S14875
Victor C Kok, Chien-Kuan Lee, Jorng-Tzong Horng, Che-Chen Lin, Fung-Chang Sung
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引用次数: 2

摘要

简介:与自身免疫性溶血性贫血(AIHA)不同,非自身免疫性溶血性贫血(non-AIHA)的病因学研究文献很少。非aiha在不同地理区域的发病率和流行程度在很大程度上是未知的,这可能是由于缺乏前瞻性调查和不同地理区域的不同病因概况。我们的目的是从台湾全国人口为基础的行政索赔数据库中研究非遗传性非aiha的真实病因或机制。研究对象与方法:本研究采用台湾全民健保研究资料库。研究对象为全台湾2,300万参保人口,包括儿童及成人病患的住院理赔记录。从2002年到2008年,我们检索了3903例获得性溶血性贫血住院治疗后出院的无既往恶性肿瘤患者,其在出院诊断中定义为编码,包含ICD-9-CM代码283。相比之下,ICD-9-CM代码282和所有子代码为遗传性溶血性贫血。结果:AIHA占总病例的32%。2657例非aiha患者中,机械性或微血管病变机制占19%;溶血性尿毒症综合征(HUS) 4%,突发性夜间血红蛋白尿(PNH)和三月血红蛋白尿(7%)等外因溶血导致的血红蛋白尿,慢性特发性溶血性贫血或其他未指明的非aiha 69%。我们进一步研究了这组非遗传性外源性非aiha患者的特定病因或机制(n = 2657)。解释疾病状态或条件为脾肿大;酒精使用障碍(骨刺细胞溶血);心脏瓣膜假体;恶性高血压;弥散性血管内凝血;输血反应;登革热引起的溶血性贫血;直接寄生作用;被蛇、蜥蜴或蜘蛛咬伤;内毒素机制的威尔逊氏病所有这些病例可解释34.6%的非遗传性外源性非aiha病例。碎片性溶血(溶血性尿毒综合征、心脏瓣膜假体、恶性高血压、弥散性血管内凝血)占非aiha住院非肿瘤性疾病患者的7.4%。结论:本文首次明确指出,在人口2300多万的台湾,7年间非肿瘤性溶血性尿毒综合征住院病例为110例,年均16例。虽然非aiha的病因在文献中已被熟知和描述,但本工作增加了台湾非aiha各种病因的统计百分比。
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Reappraisal of the etiology of extracorpuscular non-autoimmune acquired hemolytic anemia in 2657 hospitalized patients with non-neoplastic disease.

Introduction: Unlike autoimmune hemolytic anemia (AIHA), literature on the etiological study of non-autoimmune hemolytic anemia (non-AIHA) is scarce. The incidence and prevalence of non-AIHA in different geographic regions are largely unknown perhaps owing to the lack of perspective investigation and different profiles of etiologies from different geographic regions. We aimed to examine the real-world etiology or mechanisms of the non-hereditary non-AIHA from a nationwide population-based administrative claim database in Taiwan.

Patients and methods: The National Health Insurance Research Database of Taiwan was adopted for this research. The studied population was total inpatient claim records including both pediatric and adult patients, contributed by a population of 23 million insured individuals in Taiwan. From 2002 to 2008, we retrieved 3,903 patients having no pre-existing malignancy discharged after inpatient management for acquired hemolytic anemia, which was defined as coding in discharge diagnoses containing ICD-9-CM code 283. By contrast, ICD-9-CM code 282 and all of the sub-codes are for hereditary hemolytic anemias.

Results: AIHA accounted for 32% of the total cases. Among 2,657 patients with non-AIHA, mechanical or microangiopathic mechanism accounted for 19% of cases; hemolytic-uremic syndrome (HUS) 4%, hemoglobinuria because of hemolysis from external causes such as paroxysmal nocturnal hemoglobinuria (PNH) and march hemoglobinuria 7%, and chronic idiopathic hemolytic anemia or other unspecified non-AIHA 69%. We looked further for specific etiology or mechanism for this group of patients with non-hereditary extrinsic non-AIHA (n = 2,657). The explanatory disease states or conditions were splenomegaly; alcohol use disorder (spur cell hemolysis); heart-valve prosthesis; malignant hypertension; disseminated intravascular coagulation; transfusion reaction; dengue fever-induced hemolytic anemia; direct parasitization; snake, lizard, or spider bite; and Wilson's disease with internal toxin mechanism. All these cases can explain up to 34.6% of all the non-hereditary extrinsic non-AIHA cases. Fragmentation hemolysis (HUS, heart-valve prosthesis, malignant hypertension, and disseminated intravascular coagulation) accounted for 7.4% of non-AIHA hospitalized patients with non-neoplastic disease.

Conclusions: This article is the first one to clearly demonstrate that the non-neoplastic-induced HUS requiring hospitalization cases in Taiwan, which has a population of over 23 million were 110 over a span of seven years, 16 cases per year. Although the etiologies of non-AIHA are well known and described in the literature, this work added the statistical percentages of the various etiologies of non-AIHA in Taiwan.

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