S'abonner

Defective actin accumulation impairs human natural killer cell function in patients with dedicator of cytokinesis 8 deficiency - 27/02/13

Doi : 10.1016/j.jaci.2012.12.1568 
Melissa C. Mizesko, MD a, b, , Pinaki P. Banerjee, PhD a, b, , Linda Monaco-Shawver, BA c, , Emily M. Mace, PhD a, b, William E. Bernal, MD c, Julie Sawalle-Belohradsky d, Bernd H. Belohradsky, MD d, Valerie Heinz d, Alexandra F. Freeman, MD e, Kathleen E. Sullivan, MD, PhD c, Steven M. Holland, MD e, Troy R. Torgerson, MD, PhD f, Waleed Al-Herz, MD g, Janet Chou, MD h, Imelda C. Hanson, MD a, b, Michael H. Albert, MD d, Raif S. Geha, MD h, Ellen D. Renner, MD d, Jordan S. Orange, MD, PhD a, b,
a Baylor College of Medicine, Houston, Tex 
b Texas Children’s Hospital, Houston, Tex 
c Children’s Hospital of Philadelphia Research Institute, Philadelphia, Pa 
d University Children’s Hospital, Ludwig-Maximilians-Universität, Munich, Germany 
e National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Md 
f University of Washington and Seattle Children’s Hospital, Seattle, Wash 
g Pediatrics Department, Faculty of Medicine, Kuwait University, Kuwait City, Kuwait 
h Boston Children’s Hospital, Boston, Mass 

Corresponding author: Jordan S. Orange, MD, PhD, Immunology, Allergy, and Rheumatology, Texas Children’s Hospital, Baylor College of Medicine, 1102 Bates Ave, Suite 330, Houston, TX 77030-2399.

Abstract

Background

Dedicator of cytokinesis 8 (DOCK8) mutations are responsible for a rare primary combined immunodeficiency syndrome associated with severe cutaneous viral infections, increased IgE levels, autoimmunity, and malignancy. Natural killer (NK) cells are essential for tumor surveillance and defense against virally infected cells. NK cell function relies on Wiskott-Aldrich syndrome protein for filamentous actin (F-actin) accumulation at the lytic NK cell immunologic synapse. DOCK8 activates cell division cycle 42, which, together with Wiskott-Aldrich syndrome protein, coordinates F-actin reorganization. Although abnormalities in T- and B-cell function have been described in DOCK8-deficient patients, the role of NK cells in this disease is unclear.

Objectives

We sought to understand the role of DOCK8 in NK cell function to determine whether NK cell abnormalities explain the pathogenesis of the clinical syndrome of DOCK8 deficiency.

Methods

A cohort of DOCK8-deficient patients was assembled, and patients’ NK cells, as well as NK cell lines with stably reduced DOCK8 expression, were studied. NK cell cytotoxicity, F-actin content, and lytic immunologic synapse formation were measured.

Results

DOCK8-deficient patients’ NK cells and DOCK8 knockdown cell lines all had decreased NK cell cytotoxicity, which could not be restored after IL-2 stimulation. Importantly, DOCK8 deficiency impaired F-actin accumulation at the lytic immunologic synapse without affecting overall NK cell F-actin content.

Conclusions

DOCK8 deficiency results in severely impaired NK cell function because of an inability to form a mature lytic immunologic synapse through targeted synaptic F-actin accumulation. This defect might underlie and explain important attributes of the DOCK8 deficiency clinical syndrome, including the unusual susceptibility to viral infection and malignancy.

Le texte complet de cet article est disponible en PDF.

Key words : DOCK8 deficiency, natural killer cells, actin, cytotoxicity, immunologic synapse

Abbreviations used : Cdc42, DOCK8, F-actin, HIES, IS, MTOC, NK, shRNA, STAT3, WAS, WASp


Plan


 Supported by National Institutes of Health (NIH)/National Institute of Allergy and Infectious Diseases grant R01067946 (to J.S.O.), the German Research Foundation (DFG RE2799/3-1) and a Fritz-Thyssen research foundation grant (Az. 10.07.1.159; to E.D.R.); and the Dubai-Harvard Foundation of Medical Research, the Jeffrey Modell Foundation, “Role of TACI Mutations in CVID,” 5P01AI076210-04, NIH, and “Combined SNP analysis and whole genome sequencing to discover immunodeficiency genes,” 5R03AI094017-02, NIH (to R.S.G.).
 Disclosure of potential conflict of interest: M. C. Mizesko has received grants from the National Institutes of Health (NIH). L. Monaco-Shawver has received grants from the NIH. T. R. Torgerson has consulted for Baxter Biosciences; has grants/grants pending from Baxter Biosciences and CSL Behring; has received payment for lectures, including service on speakers’ bureaus for Baxter Biosciences; has received royalties from New England Biolabs; and has received payment for development of Educational Presentations from Baxter Biosciences. J. Chou is employed by Boston Children’s Hospital and has grants/grants pending from the NIH. R. S. Geha has received grants from the NIH. E. D. Renner has received grant money from DFG and the Fritz-Thyssen Foundation. J. S. Orange has received grants from the NIH; has consulted for Baxter Biosciences on lg therapies, CSL Bhering on lg therapies, Grifols on lg therapies, Octapharma USA on the Grants Review Committee, Cangene on lg therapy, and IBT reference laboratories on immunology; has received payment for lectures, including service on speakers’ bureaus for Baxter Healthcare; has received royalties from Unimed Publishers for a book on immunoglobulins; and has received payment for development of educational presentations from CSL Bhering for a presentation on lg therapy. The rest of the authors declare that they have no relevant conflicts of interest.


© 2013  Publié par Elsevier Masson SAS.
Ajouter à ma bibliothèque Retirer de ma bibliothèque Imprimer
Export

    Export citations

  • Fichier

  • Contenu

Vol 131 - N° 3

P. 840-848 - mars 2013 Retour au numéro
Article précédent Article précédent
  • Thymic function in MHC class II–deficient patients
  • Atar Lev, Amos J. Simon, Arnon Broides, Jacob Levi, Ben Zion Garty, Ester Rosenthal, Ninette Amariglio, Gideon Rechavi, Raz Somech
| Article suivant Article suivant
  • The innate antiviral response upregulates IL-13 receptor ⍺2 in bronchial fibroblasts
  • Gemma Campbell-Harding, Hannah Sawkins, Nicole Bedke, Stephen T. Holgate, Donna E. Davies, Allison-Lynn Andrews

Bienvenue sur EM-consulte, la référence des professionnels de santé.
L’accès au texte intégral de cet article nécessite un abonnement.

Déjà abonné à cette revue ?

Mon compte


Plateformes Elsevier Masson

Déclaration CNIL

EM-CONSULTE.COM est déclaré à la CNIL, déclaration n° 1286925.

En application de la loi nº78-17 du 6 janvier 1978 relative à l'informatique, aux fichiers et aux libertés, vous disposez des droits d'opposition (art.26 de la loi), d'accès (art.34 à 38 de la loi), et de rectification (art.36 de la loi) des données vous concernant. Ainsi, vous pouvez exiger que soient rectifiées, complétées, clarifiées, mises à jour ou effacées les informations vous concernant qui sont inexactes, incomplètes, équivoques, périmées ou dont la collecte ou l'utilisation ou la conservation est interdite.
Les informations personnelles concernant les visiteurs de notre site, y compris leur identité, sont confidentielles.
Le responsable du site s'engage sur l'honneur à respecter les conditions légales de confidentialité applicables en France et à ne pas divulguer ces informations à des tiers.


Tout le contenu de ce site: Copyright © 2024 Elsevier, ses concédants de licence et ses contributeurs. Tout les droits sont réservés, y compris ceux relatifs à l'exploration de textes et de données, a la formation en IA et aux technologies similaires. Pour tout contenu en libre accès, les conditions de licence Creative Commons s'appliquent.