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北美家族性噬血细胞性淋巴组织细胞增生症的 STX11 突变与临床表型。

STX11 mutations and clinical phenotypes of familial hemophagocytic lymphohistiocytosis in North America.

机构信息

Division of Bone Marrow Transplant and Immune Deficiency, Cincinnati Children's Hospital Medical Center, Cincinnati, Ohio 45229, USA.

出版信息

Pediatr Blood Cancer. 2010 Jul 15;55(1):134-40. doi: 10.1002/pbc.22499.

DOI:10.1002/pbc.22499
PMID:20486178
Abstract

BACKGROUND

Mutations in STX11 are responsible for Familial Hemophagocytic Lymphohistiocytosis (FHLH) type 4, a rare primary immunodeficiency which has previously been observed only in patients of Kurdish, Turkish, and Lebanese ethnic background.

METHODS

We reviewed our experience with STX11 mutations among North American patients and studied the impact of patient mutations upon syntaxin 11 expression and NK cell function.

RESULTS

Between 2007 and 2008, 243 patients with HLH (lacking disease-causing mutations in PRF1 and UNC13D) were referred for STX11 mutational analysis. We observed 1 novel homozygous nonsense mutation, 73 G > T (E25X), occurring in Hispanic siblings, and 2 novel biallelic heterozygous missense mutations, 106G > C (E36Q) and 616G > A (E206K), occurring in 1 Caucasian patient. The N-terminal nonsense mutation resulted in absence of detectable syntaxin 11 and abrogation of in vitro NK cell degranulation and function, while the biallelic heterozygous missense mutations resulted in detectable mutated syntaxin 11 and preservation of in vitro NK cell degranulation and cytotoxicity. The two sibling patients with the nonsense mutations presented with HLH during infancy, whereas the patient with biallelic heterozygous missense mutations presented at 5 years of age.

CONCLUSION

We conclude that mutations in STX11 are responsible for HLH in approximately 1% of North American patients and can cause variable defects in syntaxin 11 expression and function with resultant impact on clinical phenotype.

摘要

背景

STX11 突变可导致家族性噬血细胞性淋巴组织细胞增生症(FHLH)4 型,这是一种罕见的原发性免疫缺陷病,此前仅在库尔德、土耳其和黎巴嫩血统的患者中观察到。

方法

我们回顾了我们在北美患者中对 STX11 突变的经验,并研究了患者突变对 syntaxin 11 表达和 NK 细胞功能的影响。

结果

在 2007 年至 2008 年间,我们对 243 名缺乏 PRF1 和 UNC13D 致病突变的 HLH 患者进行了 STX11 突变分析。我们观察到 1 个新的纯合无义突变,73G>T(E25X),发生在西班牙裔兄弟姐妹中,以及 2 个新的双等位基因杂合错义突变,106G>C(E36Q)和 616G>A(E206K),发生在 1 名白种人患者中。N 端无义突变导致无法检测到 syntaxin 11,并阻断体外 NK 细胞脱颗粒和功能,而双等位基因杂合错义突变导致可检测到突变的 syntaxin 11,并保留体外 NK 细胞脱颗粒和细胞毒性。携带无义突变的 2 名同胞患者在婴儿期出现 HLH,而携带双等位基因杂合错义突变的患者在 5 岁时出现。

结论

我们得出结论,STX11 突变导致大约 1%的北美患者发生 HLH,并可导致 syntaxin 11 表达和功能的不同缺陷,从而影响临床表型。

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