Dominant-negative SERPING1 variants cause intracellular retention of C1 inhibitor in hereditary angioedema
Didde Haslund, … , Lene N. Nejsum, Jacob Giehm Mikkelsen
Didde Haslund, … , Lene N. Nejsum, Jacob Giehm Mikkelsen
Published November 6, 2018
Citation Information: J Clin Invest. 2019;129(1):388-405. https://doi.org/10.1172/JCI98869.
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Research Article Cell biology Genetics

Dominant-negative SERPING1 variants cause intracellular retention of C1 inhibitor in hereditary angioedema

Abstract

Hereditary angioedema (HAE) is an autosomal dominant disease characterized by recurrent edema attacks associated with morbidity and mortality. HAE results from variations in the SERPING1 gene that encodes the C1 inhibitor (C1INH), a serine protease inhibitor (serpin). Reduced plasma levels of C1INH lead to enhanced activation of the contact system, triggering high levels of bradykinin and increased vascular permeability, but the cellular mechanisms leading to low C1INH levels (20%–30% of normal) in heterozygous HAE type I patients remain obscure. Here, we showed that C1INH encoded by a subset of HAE-causing SERPING1 alleles affected secretion of normal C1INH protein in a dominant-negative fashion by triggering formation of protein-protein interactions between normal and mutant C1INH, leading to the creation of larger intracellular C1INH aggregates that were trapped in the endoplasmic reticulum (ER). Notably, intracellular aggregation of C1INH and ER abnormality were observed in fibroblasts from a heterozygous carrier of a dominant-negative SERPING1 gene variant, but the condition was ameliorated by viral delivery of the SERPING1 gene. Collectively, our data link abnormal accumulation of serpins, a hallmark of serpinopathies, with dominant-negative disease mechanisms affecting C1INH plasma levels in HAE type I patients, and may pave the way for new treatments of HAE.

Authors

Didde Haslund, Laura Barrett Ryø, Sara Seidelin Majidi, Iben Rose, Kristian Alsbjerg Skipper, Tue Fryland, Anja Bille Bohn, Claus Koch, Martin K. Thomsen, Yaseelan Palarasah, Thomas J. Corydon, Anette Bygum, Lene N. Nejsum, Jacob Giehm Mikkelsen

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Figure 9

Formation of C1INH aggregates containing associated normal and mutant C1INH induced by dominant-negative SERPING1 gene variants causing HAE.

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Formation of C1INH aggregates containing associated normal and mutant C1...
(A) Live widefield microscopy of HeLa cells cultured for 48 hours after cotransfection with 450 ng pSERPING1[WT]-mCherry and 450 ng pSERPING1[Variant]. Aggregates are indicated with arrows. Scale bars: 10 μm. (B) Western blot analysis of medium, soluble and insoluble C1INH derived from HeLa cells cultured for 72 hours after cotransfection with 450 ng pSERPING1[WT]-HA and 450 ng pSERPING1[Variant]. The experiment was carried out as described in Figure 6, B and C. (C) Coimmunoprecipitation on cell lysate from HeLa cells cultured for 48 hours after cotransfection with 20 μg pSERPING1[WT]-V5 and 20 μg pSERPING1[Variant]-HA. The experiment was carried out as described in Figure 6D. (A and B) Data are representative of findings from more than 3 biological replicates and similar results were seen in at least 2 independent experiments. Transfections were carried out in triplicate (n = 3; B) or duplicate (n = 2; C).