Aberrant subcellular targeting of the G185R neutrophil elastase mutant associated with severe congenital neutropenia induces premature apoptosis of differentiating promyelocytes

Massullo, Pam; Druhan, Lawrence J.; Bunnell, Bruce A.; Hunter, Melissa; Robinson, John M.; Marsh, Clay B.; Avalos, Belinda R.

doi:10.1182/blood-2004-07-2618

Cited by 57 publications

(62 citation statements)

References 45 publications

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“…Effects on proteolytic activity, on cellular trafficking and on unfolded protein response (UPR) have been demonstrated only for subgroups of ELANE mutations, respectively. [11][12][13][14] Furthermore, other ELANE mutations described as causative for congenital neutropenia, e.g. p.Val72Met 1 were also categorized as benign by the prediction algorithms.…”

Section: Resultsmentioning

confidence: 99%

Digenic mutations in severe congenital neutropenia

Germeshausen¹,

Zeidler²,

Stuhrmann³

et al. 2010

Haematologica

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Severe congenital neutropenia a clinically and genetically heterogeneous disorder. Mutations in different genes have been described as causative for severe neutropenia, e.g. ELANE, HAX1 and G6PC3. Although congenital neutropenia is considered to be a group of monogenic disorders, the phenotypic heterogeneity even within the yet defined genetic subtypes points to additional genetic and/or epigenetic influences on the disease phenotype. We describe congenital neutropenia patients with mutations in two candidate genes each, including 6 novel mutations. Two of them had a heterozygous ELANE mutation combined with a homozygous mutation in G6PC3 or HAX1, respectively. The other 2 patients combined homozygous or compound heterozygous mutations in G6PC3 or HAX1 with a heterozygous mutation in the respective other gene. Our results suggest that digenicity may underlie this disorder of myelopoiesis at least in some congenital neutropenia patients.

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Section: Resultsmentioning

confidence: 99%

Digenic mutations in severe congenital neutropenia

Germeshausen¹,

Zeidler²,

Stuhrmann³

et al. 2010

Haematologica

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“…[54][55][56] There have been several contradicting reports on disturbances in the subcellular localization of neutrophil elastase caused by mutations associated with CN or SCN. 10,57 It has particularly been suggested that mutations in neutrophil elastase affect the sorting to granules via disorganization of putative transmembrane and cytosolic domains. 58 Our finding that lack of serglycin completely prevents granule localization of elastase argues against a significant role of putative transmembrane and cytosolic domains of neutrophil elastase in granule targeting.…”

Section: Discussionmentioning

confidence: 99%

Neutrophil elastase depends on serglycin proteoglycan for localization in granules

Niemann

Åbrink

Pejler

et al. 2007

Blood

101

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Granule proteins play a major role in bacterial killing by neutrophils. Serglycin proteoglycan, the major intracellular proteoglycan of hematopoietic cells, has been proposed to play a role in sorting and packing of granule proteins. We examined the content of major neutrophil granule proteins in serglycin knockout mice and found neutrophil elastase absent from mature neutrophils as shown by activity assay, Western blotting, and immunocytochemistry, whereas neutrophil elastase mRNA was present.

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“…This might be due to inappropriate ANC monitoring, G-CSF treatment related cycle modification, incomplete mutation spectrum data, phenotype diversification by modifier genes and additional somatic mutations, especially in the colony stimulating factor 3 receptor gene (CSF3R) [11][12][13][14]15 16,17]. The monomeric serine chymotryptic-type protease neutrophil elastase is a major component of neutrophil granulocyte azurophilic granules and is named after its first known substrate elastin [129].…”

Section: Elane Deficiencymentioning

confidence: 99%