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Neuropathology of McLeod Syndrome.麦克劳德综合征的神经病理学
Mov Disord. 2022 Mar;37(3):644-646. doi: 10.1002/mds.28882. Epub 2021 Dec 16.
2
The tertiary structure of the human Xkr8-Basigin complex that scrambles phospholipids at plasma membranes.人源 Xkr8-Basigin 复合物在质膜上扰乱磷脂的三级结构。
Nat Struct Mol Biol. 2021 Oct;28(10):825-834. doi: 10.1038/s41594-021-00665-8. Epub 2021 Oct 8.
3
Three new XK alleles; two associated with a McLeod RBC phenotype.三个新的XK等位基因;两个与麦克劳德红细胞表型相关。
Transfusion. 2021 Oct;61(10):E69-E70. doi: 10.1111/trf.16650. Epub 2021 Sep 6.
4
Brain F-18 FDG and F-18 FP-CIT PET/CT Findings of c.856_860delCTCTA Mutation McLeod Syndrome.脑 F-18 FDG 和 F-18 FP-CIT PET/CT 在 McLeod 综合征 c.856_860delCTCTA 突变中的表现。
Cogn Behav Neurol. 2021 Sep 2;34(3):207-211. doi: 10.1097/WNN.0000000000000267.
5
Cryo-EM structures of the caspase-activated protein XKR9 involved in apoptotic lipid scrambling.凋亡脂质重排相关的半胱天冬酶激活蛋白 XKR9 的冷冻电镜结构。
Elife. 2021 Jul 15;10:e69800. doi: 10.7554/eLife.69800.
6
Insights into VPS13 properties and function reveal a new mechanism of eukaryotic lipid transport.深入了解 VPS13 的特性和功能揭示了真核生物脂质运输的新机制。
Biochim Biophys Acta Mol Cell Biol Lipids. 2021 Oct;1866(10):159003. doi: 10.1016/j.bbalip.2021.159003. Epub 2021 Jul 1.
7
Effect of cryopreservation on a rare McLeod donor red blood cell concentrate.冷冻保存对罕见的 McLeod 供者红细胞浓缩物的影响。
Immunohematology. 2021 Jun;37(2):78-83. doi: 10.21307/immunohematology-2021-012.
8
Cardiac manifestation is evident in chorea-acanthocytosis but different from McLeod syndrome.心脏表现明显在舞蹈棘红细胞增多症,但与 McLeod 综合征不同。
Parkinsonism Relat Disord. 2021 Jul;88:90-95. doi: 10.1016/j.parkreldis.2021.05.015. Epub 2021 May 24.
9
Targeting Lyn Kinase in Chorea-Acanthocytosis: A Translational Treatment Approach in a Rare Disease.针对舞蹈病-棘红细胞增多症中的Lyn激酶:一种罕见病的转化治疗方法
J Pers Med. 2021 May 10;11(5):392. doi: 10.3390/jpm11050392.
10
The Erythrocyte Sedimentation Rate and Its Relation to Cell Shape and Rigidity of Red Blood Cells from Chorea-Acanthocytosis Patients in an Off-Label Treatment with Dasatinib.红细胞沉降率及其与舞蹈棘红细胞增多症患者在达沙替尼标签外治疗时红细胞形状和刚性的关系。
Biomolecules. 2021 May 12;11(5):727. doi: 10.3390/biom11050727.

与XK相关的麦克劳德综合征:非血液学表现及其与VPS13A疾病的关系

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

作者信息

Peikert Kevin, Hermann Andreas, Danek Adrian

机构信息

Translational Neurodegeneration Section "Albrecht Kossel", Department of Neurology, University Medical Center Rostock, University of Rostock, Rostock, Germany.

DZNE, German Center for Neurodegenerative Diseases, Research Site Rostock/Greifswald, Rostock, Germany.

出版信息

Transfus Med Hemother. 2022 Jan 25;49(1):4-12. doi: 10.1159/000521417. eCollection 2022 Feb.

DOI:10.1159/000521417
PMID:35221863
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8832239/
Abstract

BACKGROUND

McLeod syndrome (MLS) is an X-linked multisystemic progressive disorder caused by loss of function mutations in the 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 (or , 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 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 , , and 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.

摘要

背景

麦克劳德综合征(MLS)是一种X连锁多系统进行性疾病,由该基因的功能丧失突变引起。MLS患者缺乏Kx抗原这一罕见血型表型,因存在输血并发症风险,需要专业输血机构的支持。几乎所有患者都会出现红细胞棘形红细胞增多症。MLS的非血液学表现与常染色体隐性疾病VPS13A病(舞蹈病-棘红细胞增多症)非常相似。除棘形红细胞增多症外,它们共有的表型还包括舞蹈病和肌张力障碍等运动障碍、癫痫、周围神经病变以及肌肉受累,通常伴有肌酸激酶(CK)升高,包括心肌病。

总结

在本综述中,我们将MLS的非血液学表现与VPS13A病的表现进行了比较。虽然存在许多相似之处,但诸如遗传方式、性别分布、发病年龄、心脏受累严重程度、喂养性肌张力障碍或不自主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。麦克劳德-凯尔表型的免疫血液学证明或(或分别)致病突变的检测是区分的金标准。“神经棘红细胞增多症”常被用作一个总体术语,但可能会产生误导,因为该术语并不指一种明确的疾病实体。如果继续使用该术语,绝不能妨碍临床医生根据分子学发现寻求最终诊断。MLS和VPS13A病在临床上的相似性长期以来表明它们有一些共同的病理生理学机制。最近有人提出XK(麦克劳德蛋白)与VPS13A基因产物舞蹈蛋白之间存在分子相互作用的证据:XK与舞蹈蛋白/VPS13A形成复合物,VPS13A是一种位于各种膜接触位点的大量脂质转运蛋白。XK在该复合物中的具体作用需要进一步阐明。大量脂质转运受损似乎是MLS和VPS13A病的共同特征。随着时间的推移,可能会有更多疾病被纳入“大量脂质转运疾病”,比如最近发现的由、和基因的突变引起的疾病。

关键信息

(1)被诊断为罕见红细胞麦克劳德表型(麦克劳德综合征,MLS)的患者,因其血液学和非血液学疾病表现,需要输血医学专家、神经科医生和心脏病专家进行多学科协作。(2)MLS和VPS13A病在表型上的相似性,常常导致混淆或诊断深度不足(在“神经棘红细胞增多症 ”这一标签下),其基础是各自的蛋白质XK和舞蹈蛋白在大量脂质转运的细胞机制内相互作用。(3)总体而言,“大量脂质转运疾病”这一术语似乎有助于对一组疾病进行进一步研究,这些疾病不仅可能有共同的病理生理学机制,还可能有共同的治疗方法。