Human HOIP and LUBAC Deficiency Underlies Autoinflammation, Immunodeficiency, Amylopectinosis, and Lymphangiectasia

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 2015 May 27

PMID 26008899

Citations 133

Authors

Bertrand Boisson

Emmanuel Laplantine

Kerry Dobbs

Aurelie Cobat

Nadine Tarantino

Melissa Hazen

Hart G W Lidov

Gregory Hopkins

Likun Du

Aziz Belkadi

Maya Chrabieh

Yuval Itan

Capucine Picard

Jean-Christophe Fournet

Hermann Eibel

Erdyni Tsitsikov

Sung-Yun Pai

Laurent Abel

Waleed Al-Herz

Jean-Laurent Casanova

Alain Israel

Luigi D Notarangelo

Affiliations

Soon will be listed here.

Abstract

Inherited, complete deficiency of human HOIL-1, a component of the linear ubiquitination chain assembly complex (LUBAC), underlies autoinflammation, infections, and amylopectinosis. We report the clinical description and molecular analysis of a novel inherited disorder of the human LUBAC complex. A patient with multiorgan autoinflammation, combined immunodeficiency, subclinical amylopectinosis, and systemic lymphangiectasia, is homozygous for a mutation in HOIP, the gene encoding the catalytic component of LUBAC. The missense allele (L72P, in the PUB domain) is at least severely hypomorphic, as it impairs HOIP expression and destabilizes the whole LUBAC complex. Linear ubiquitination and NF-κB activation are impaired in the patient's fibroblasts stimulated by IL-1β or TNF. In contrast, the patient's monocytes respond to IL-1β more vigorously than control monocytes. However, the activation and differentiation of the patient's B cells are impaired in response to CD40 engagement. These cellular and clinical phenotypes largely overlap those of HOIL-1-deficient patients. Clinical differences between HOIL-1- and HOIP-mutated patients may result from differences between the mutations, the loci, or other factors. Our findings show that human HOIP is essential for the assembly and function of LUBAC and for various processes governing inflammation and immunity in both hematopoietic and nonhematopoietic cells.

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