Large deletions and point mutations involving the dedicator of cytokinesis 8 (DOCK8) in the autosomal-recessive form of hyper-IgE syndrome

被引：405

作者：

Engelhardt, Karin R. ^{[1
,2
]}

McGhee, Sean ^{[3
]}

Winkler, Sabine ^{[1
,2
]}

Sassi, Atfa ^{[4
]}

Woellner, Cristina ^{[1
,2
]}

Lopez-Herrera, Gabriela ^{[1
,2
]}

Chen, Andrew ^{[3
]}

Kim, Hong Sook ^{[3
]}

Lloret, Maria Garcia ^{[3
]}

Schulze, Ilka ^{[5
]}

Ehl, Stephan ^{[5
]}

Thiel, Jens ^{[5
]}

Pfeifer, Dietmar ^{[6
]}

Veelken, Hendrik ^{[6
]}

Niehues, Tim ^{[7
]}

Siepermann, Kathrin ^{[7
]}

Weinspach, Sebastian ^{[8
]}

Reisli, Ismail ^{[9
]}

Keles, Sevgi ^{[9
]}

Genel, Ferah ^{[10
]}

Kutuculer, Necil ^{[11
]}

Camcioglu, Yildiz ^{[12
]}

Somer, Ayper ^{[13
]}

Karakoc-Aydiner, Elif ^{[14
]}

Barlan, Isil ^{[14
]}

Gennery, Andrew ^{[15
]}

Metin, Ayse ^{[16
]}

Degerliyurt, Aydan ^{[16
]}

Pietrogrande, Maria C. ^{[17
]}

Yeganeh, Mehdi ^{[18
]}

Baz, Zeina ^{[19
]}

Al-Tamemi, Salem ^{[20
]}

Klein, Christoph ^{[21
]}

Puck, Jennifer M. ^{[22
]}

Holland, Steven M. ^{[23
,24
,25
,26
,27
]}

McCabe, Edward R. B.

Grimbacher, Bodo ^{[1
,2
]}

Chatila, Talal A. ^{[3
]}

机构：

[1] Royal Free Hosp, Dept Immunol & Mol Pathol, London NW3 2QG, England

[2] UCL, London NW3 2QG, England

[3] Univ Calif Los Angeles, David Geffen Sch Med, Div Immunol Allergy & Rheumatol, Dept Pediat, Los Angeles, CA 90095 USA

[4] Inst Pasteur Tunis, Lab Immunol Vaccinol & Genet Mol, Tunis, Tunisia

[5] Univ Med Ctr Freiburg, Ctr Chron Immunodeficiency, Freiburg, Germany

[6] Univ Med Ctr Freiburg, Dept Hematol Oncol, Freiburg, Germany

[7] HELIOS Klinikum Krefeld, Zentrum Kinder & Jugendmed, Krefeld, Germany

[8] Univ Dusseldorf, Dept Pediat Oncol Hematol & Clin Immunol, Ctr Child & Adolescent Med, Dusseldorf, Germany

[9] Selcuk Univ, Div Pediat Allergy & Immunol, Konya, Turkey

[10] Behcet Uz State Hosp, Div Pediat Immunol, Izmir, Turkey

[11] Ege Univ, Fac Med, Dept Pediat, Izmir, Turkey

[12] Istanbul Univ, Cerrahpasa Med Fac, Div Pediat Allergy Immunol & Infect Dis, Istanbul, Turkey

[13] Istanbul Univ, Istanbul Fac Med, Div Infect Dis & Immunol, Istanbul, Turkey

[14] Marmara Univ, Div Pediat Allergy & Immunol, Istanbul, Turkey

[15] Newcastle Univ, Inst Cellular Med, Newcastle Upon Tyne NE1 7RU, Tyne & Wear, England

[16] SB Ankara Diskapi Childrens Hosp, Pediat Immunol Unit, Ankara, Turkey

[17] Univ Milan, Fdn IRCCS Policlin Milano, Dept Maternal & Pediat Sci, Milan, Italy

[18] Univ Tehran Med Sci, Childrens Med Ctr, Immunol Asthma & Allergy Res Inst, Tehran, Iran

[19] Univ Med Ctr, St George Hosp, Dept Pediat, Beirut, Lebanon

[20] Sultan Qaboos Univ, Dept Pediat, Muscat, Oman

[21] Hannover Biomed Res Sch, Dept Pediat Hematol Oncol, Hannover, Germany

[22] Univ Calif San Francisco, San Francisco, CA 94143 USA

[23] NIAID, Lab Clin Infect Dis, NIH, Bethesda, MD 20892 USA

[24] Univ Calif Los Angeles, Dept Pediat, Los Angeles, CA 90024 USA

[25] Univ Calif Los Angeles, Dept Human Genet, Los Angeles, CA USA

[26] Univ Calif Los Angeles, Dept Bioengn, Los Angeles, CA USA

[27] Univ Calif Los Angeles, Ctr Soc & Genet, Los Angeles, CA USA

来源：

JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY | 2009年 / 124卷 / 06期

基金：

美国国家卫生研究院;

关键词：

Autosomal recessive hyper-IgE syndrome; human gene mutation; DOCK8; primary immunodeficiency; molluscum contagiosum; recurrent infection; T cells; T(H)17 cells; eosinophils; IgE regulation; copy number variations; genomic deletions; IDENTIFICATION; REARRANGEMENTS; GENOME;

D O I：

10.1016/j.jaci.2009.10.038

中图分类号：

R392 [医学免疫学];

学科分类号：

100102 ;

摘要：

Background: The genetic etiologies of the hyper-IgE syndromes are diverse. Approximately 60% to 70% of patients with hyper-IgE syndrome have dominant mutations in STAT3, and a single patient was reported to have a homozygous TYK2 mutation. In the remaining patients with hyper-IgE syndrome, the genetic etiology has not yet been identified. Objectives: We aimed to identify a gene that is mutated or deleted in autosomal recessive hyper-IgE syndrome. Methods: We performed genome-wide single nucleotide polymorphism analysis for 9 patients with autosomal-recessive hyper-IgE syndrome to locate copy number variations and homozygous haplotypes. Homozygosity mapping was performed with 12 patients from 7 additional families. The candidate gene was analyzed by genomic and cDNA sequencing to identify causative alleles in a total of 27 patients with autosomal-recessive hyper-IgE syndrome. Results: Subtelomeric biallelic microdeletions were identified in 5 patients at the terminus of chromosome 9p. In all 5 patients, the deleted interval involved dedicator of cytokinesis 8 (DOCK8), encoding a protein implicated in the regulation of the actin cytoskeleton. Sequencing of patients without large deletions revealed 16 patients from 9 unrelated families with distinct homozygous mutations in DOCK8 causing premature termination, frameshift, splice site disruption, and single exon deletions and microdeletions. DOCK8 deficiency was associated with impaired activation of CD4(+) and CD8(+)T cells. Conclusion: Autosomal-recessive mutations in DOCK8 are responsible for many, although not all, cases of wautosomal-recessive hyper-IgE syndrome. DOCK8 disruption is associated with a phenotype of severe cellular immunodeficiency characterized by susceptibility to viral infections, atopic eczema, defective T-cell activation and T(H)17 cell differentiation, and impaired eosinophil homeostasis and dysregulation of IgE. (J Allergy Clin Immunol 2009;124:1289-302.)

引用

页码：1289 / 1302

页数：14

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