Mutations in neutrophil elastase causing congenital neutropenia lead to cytoplasmic protein accumulation and induction of the unfolded protein response

Köllner, Inga; Sodeik, Beate; Schreek, Sabine; Heyn, Holger; Neuhoff, Nils von; Germeshausen, Manuela; Zeidler, Cornelia; Krüger, Martin; Schlegelberger, Brigitte; Welte, Karl; Beger, Carmela

doi:10.1182/blood-2005-11-4689

Cited by 187 publications

(191 citation statements)

References 29 publications

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“…It has been reported that induction of the endoplasmic reticulum stress (ER) response and the unfolded protein response (UPR) has been advanced as a potential explanation for the molecular pathogenesis of SCN (18,19). Thus, we examined activation of the UPR by X-box binding protein 1 (XBP-1) mRNA splicing on day 7.…”

Section: Resultsmentioning

confidence: 99%

Wnt3a stimulates maturation of impaired neutrophils developed from severe congenital neutropenia patient-derived pluripotent stem cells

Hiramoto

Ebihara

Mizoguchi

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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The derivation of induced pluripotent stem (iPS) cells from individuals of genetic disorders offers new opportunities for basic research into these diseases and the development of therapeutic compounds. Severe congenital neutropenia (SCN) is a serious disorder characterized by severe neutropenia at birth. SCN is associated with heterozygous mutations in the neutrophil elastase [elastase, neutrophil-expressed (ELANE)] gene, but the mechanisms that disrupt neutrophil development have not yet been clarified because of the current lack of an appropriate disease model. Here, we generated iPS cells from an individual with SCN (SCN-iPS cells). Granulopoiesis from SCN-iPS cells revealed neutrophil maturation arrest and little sensitivity to granulocyte-colony stimulating factor, reflecting a disease status of SCN. Molecular analysis of the granulopoiesis from the SCN-iPS cells vs. control iPS cells showed reduced expression of genes related to the wingless-type mmtv integration site family, member 3a (Wnt3a)/β-catenin pathway [e.g., lymphoid enhancer-binding factor 1], whereas Wnt3a administration induced elevation lymphoid enhancer-binding factor 1-expression and the maturation of SCN-iPS cell-derived neutrophils. These results indicate that SCN-iPS cells provide a useful disease model for SCN, and the activation of the Wnt3a/β-catenin pathway may offer a novel therapy for SCN with ELANE mutation.

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Section: Resultsmentioning

confidence: 99%

Wnt3a stimulates maturation of impaired neutrophils developed from severe congenital neutropenia patient-derived pluripotent stem cells

Hiramoto

Ebihara

Mizoguchi

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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“…De même, il n'a pas été retrouvé de corrélation entre les mutations et l'activité enzymatique de la protéine. En revanche, des anomalies de conformation de la protéine et son accumulation au niveau intracytoplasmique [8,9] ont été décrites. Un taux excessif de la protéine entraînerait une mort cellulaire par apoptose.…”

Section: Généralités Sur Les Neutropénies Congénitalesunclassified

Granulopoïèse et leucémogenèse

Donadieu

Beaupain²,

Bellanné‐Chantelot³

2008

Med Sci (Paris)

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“…These mutations are now hypothesized to cause a less severe degree of accelerated apoptosis than those associated with severe congenital neutropenia. Current evidence indicates that the accelerated apoptosis of neutrophils in cyclic neutropenia is a caspase independent process [21]. Cyclic neutropenia and severe congenital neutropenia are recognized as different diseases, but the finding that mutations in the ELA-2 gene can cause both diseases prompted genotype-phenotype studies.…”

Section: Genotype-phenotype Relationshipsmentioning

confidence: 99%

“…The patterns of mutation in the two diseases shown in Figure 2. Modeling studies suggest that the mutations causing cyclic neutropenia affect the binding of neutrophil elastase to its substrates and natural inhibitors, whereas those causing congenital neutropenia may predominantly affect molecular association and folding for storage in the primary granules [21]. It is not yet clear whether specific ELA2 mutations, particularly those associated with congenital neutropenia, are associated with evolution to leukemia or if the risk of leukemia is an intrinsic risk due to more rapid turnover of progenitor cells as a response to ineffective formation of neutrophils.…”

Section: Genotype-phenotype Relationshipsmentioning

confidence: 99%

“…It is significant that the break in cell development is at the pro-myelocyte to myelocyte transition, the stage at which the enzyme neutrophil elastase is normally synthesized and packaged in the primary granules. At the cellular and molecular level, mutant neutrophil elastase triggers accelerated apoptosis, either as a direct effect of the mutant protein or secondary to the unfolded protein response with induction of caspase-independent apoptosis [18,21].…”

Section: Pathophysiologymentioning

confidence: 99%

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