XK-Associated McLeod Syndrome: Nonhematological Manifestations and Relation to VPS13A Disease

IF 1.9 4区 医学 Q3 HEMATOLOGY Transfusion Medicine and Hemotherapy Pub Date : 2022-01-25 DOI:10.1159/000521417
K. Peikert, A. Hermann, A. Danek
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引用次数: 9

Abstract

Background: McLeod syndrome (MLS) is an X-linked multisystemic progressive disorder caused by loss of function mutations in the XK gene. The rare blood group phenotype of MLS patients with absent Kx antigen requires the support of specialized transfusion institutions because of the risk of transfusion complications. Acanthocytosis of red blood cells occurs in almost all patients. Nonhematological manifestations of MLS are very similar to those of VPS13A disease (chorea-acanthocytosis), an autosomal-recessive condition. Their shared phenotype apart from acanthocytosis includes movement disorders such as chorea and dystonia, epilepsy, peripheral neuropathy, and muscle involvement, typically with creatine kinase (CK) elevation, cardiomyopathy included. Summary: In this review, we describe the nonhematological manifestations of MLS in comparison with those of VPS13A disease. While there are many similarities, differences such as mode of inheritance, sex distribution, age at manifestation, severity of heart involvement, frequency of feeding dystonia or of involuntary head drops may help to distinguish these disorders in the clinic. Immunohematological demonstration of the McLeod-Kell phenotype or detection of pathogenic mutations of XK (or VPS13A, respectively) is the gold standard for distinction. “Neuroacanthocytosis” was often used as an overarching term, but is potentially misleading, as the term does not refer to a defined disease entity. Its use, if continued, must not prevent clinicians to seek a final diagnosis on the basis of molecular findings. The clinical similarity of MLS and VPS13A disease has long suggested some shared pathophysiology. Evidence for molecular interaction between XK, the McLeod protein, and chorein, the VPS13A gene product, has recently been put forward: XK forms a complex with chorein/VPS13A, a bulk lipid transporter located at various membrane contact sites. The exact role of XK in this complex needs to be further elucidated. Impairment of bulk lipid transport appears as the common denominator of both MLS and VPS13A disease. A variety of further conditions may in time be added to the “bulk lipid transport diseases,” such as the recently recognized disorders caused by mutations in the VPS13B, VPS13C, and VPS13D genes. Key Messages: (1) Patients diagnosed with the rare red cell McLeod phenotype (McLeod syndrome, MLS) require interdisciplinary collaboration of transfusion medicine specialists, neurologists, and cardiologists for both their hematological and nonhematological disease manifestations. (2) The phenotypical similarity of MLS and VPS13A disease, often leading to either confusion or insufficient diagnostic depth (under the label of “neuroacanthocytosis”), is based on interaction of the respective proteins, XK and chorein, within the cellular machinery for bulk lipid transport. (3) Overall, the term “bulk lipid transport diseases” seems useful for further research on a group of conditions that may not only share pathophysiology, but may also share treatment approaches.
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xk相关McLeod综合征:非血液学表现及与VPS13A疾病的关系
背景:McLeod综合征(MLS)是一种由XK基因功能缺失突变引起的X连锁多系统进行性疾病。Kx抗原缺失的MLS患者的罕见血型表型需要专业输血机构的支持,因为存在输血并发症的风险。红细胞的刺突增多症几乎发生在所有患者身上。MLS的非血液学表现与VPS13A疾病(舞蹈病棘细胞增多症)非常相似,后者是一种常染色体隐性遗传疾病。除棘细胞增多症外,它们的共同表型包括运动障碍,如舞蹈病和肌张力障碍、癫痫、周围神经病变和肌肉受累,通常伴有肌酸激酶(CK)升高,包括心肌病。摘要:在这篇综述中,我们描述了MLS与VPS13A疾病的非血液学表现的比较。虽然有很多相似之处,但遗传方式、性别分布、表现时的年龄、心脏受累的严重程度、进食肌张力障碍或非自愿头部下垂的频率等差异可能有助于在临床上区分这些疾病。McLeod Kell表型的免疫血液学证明或XK(或VPS13A)致病性突变的检测是区分的金标准。“神经棘细胞增多症”经常被用作一个总体术语,但可能具有误导性,因为该术语并不是指一个定义的疾病实体。如果继续使用,一定不能阻止临床医生根据分子发现寻求最终诊断。长期以来,MLS和VPS13A疾病的临床相似性表明了一些共同的病理生理学。最近提出了McLeod蛋白XK和VPS13A基因产物舞蹈蛋白之间分子相互作用的证据:XK与舞蹈蛋白/VPS3A形成复合物,舞蹈蛋白/VPST3A是一种位于各种膜接触位点的大量脂质转运蛋白。XK在这个复合体中的确切作用还有待进一步阐明。大量脂质转运受损是MLS和VPS13A疾病的共同特征。随着时间的推移,各种进一步的疾病可能会被添加到“大量脂质转运疾病”中,例如最近发现的由VPS13B、VPS13C和VPS13D基因突变引起的疾病。关键信息:(1)被诊断为罕见红细胞McLeod表型(McLeod综合征,MLS)的患者需要输血医学专家、神经学家和心脏病学家就其血液学和非血液学疾病表现进行跨学科合作。(2) MLS和VPS13A疾病的表型相似性,通常导致混淆或诊断深度不足(被称为“神经棘细胞增多症”),是基于各自蛋白质XK和舞蹈蛋白在大量脂质转运的细胞机制内的相互作用。(3) 总的来说,“大量脂质转运疾病”一词似乎有助于对一组疾病进行进一步研究,这些疾病不仅可能具有共同的病理生理学,而且可能具有共同治疗方法。
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来源期刊
CiteScore
4.00
自引率
9.10%
发文量
47
审稿时长
6-12 weeks
期刊介绍: This journal is devoted to all areas of transfusion medicine. These include the quality and security of blood products, therapy with blood components and plasma derivatives, transfusion-related questions in transplantation, stem cell manipulation, therapeutic and diagnostic problems of homeostasis, immuno-hematological investigations, and legal aspects of the production of blood products as well as hemotherapy. Both comprehensive reviews and primary publications that detail the newest work in transfusion medicine and hemotherapy promote the international exchange of knowledge within these disciplines. Consistent with this goal, continuing clinical education is also specifically addressed.
期刊最新文献
Erratum. Autoimmune Hemolytic Anemias: Challenges in Diagnosis and Therapy. Classical Haematology: Dynamic Development at the Interface of Transfusion Medicine and Haematology. Paroxysmal Nocturnal Hemoglobinuria, Pathophysiology, Diagnostics, and Treatment. Sickle Cell Disease.
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