Misfolding of Mutated Vasopressin Causes ER-Retention and Activation of ER-Stress Markers in Neuro-2a Cells

Abstract: Summary Arginine-vasopressin (AVP) is a peptide hormone normally secreted from neuroendocrine cells via the regulated secretory pathway. In Familial Neurohypophyseal Diabetes Insipidus (FNDI), an autosomal dominant form of central diabetes insipidus, mutations of pro-vasopressin appear to accumulate in the endoplasmic reticulum (ER) causing a lack of biologically active AVP in the blood. To investigate the effect of pro-vasopressin mutations regarding intracellular functions of protein targeting and secretion,… Show more

“…To assess whether the accumulation of misfolded proteins does indeed cause UPR activation in hepatocytes, HuH7 cells transfected with either PCSK9 WT or its ER-retention variant PCSK9 Q152H were compared with cells transfected with two VP variants, VP G14R and VP G17V , known to induce ER stress in N2a cells (20,21). Consistent with previous reports, our data demonstrate that ER retention of VP leads to UPR activation as determined by immunoblotting for GRP78 and IRE1␣ ( Fig.…”

“…A well-characterized ERSD occurring in liver results from a number of established mutations in ␣ 1 -antitrypsin Z that induce ER stress, liver cirrhosis, and hepatocellular carcinoma (35,36). Additional examples affecting other tissues include arginine vasopressin mutations (G14R and G17V) in familial neurohypophyseal diabetes insipidus (20,21,37), cystic fibrosis transmembrane conductance regulator ⌬F508 in cystic fibrosis (38), thyroglobulin mutations in congenital goiter and hyperthyroidism (39), and mutations in the Notch receptor that lead to cerebral autosomal-dominant arteriopathy and leukoencephalopathy (40).…”

“…A well-described form of ERSD occurs as a result of ER arginine vasopressin (VP) retention arising from mutations such as VP G14R and VP G17V . These naturally occurring mutations play a central role in the development of familial neurohypophyseal diabetes insipidus in a manner dependent on ER stress and subsequent UPR activation (20,21). The UPR signaling cascade consists of three major transducers located at the ER membrane that are activated upon dissociation of GRP78 from their intra-ER domains.…”

“…C and D, cell viability assays were carried out on transfected HK-2 and HuH7 cells using trypan blue stain and lactate dehydrogenase assays, respectively. E, a lactate dehydrogenase assay was also carried out on cells transfected with VP G17V , a mutant known to induce ER stress as a result of ER retention (21). F, freshly isolated mouse primary hepatocytes were transfected with PCSK9 variants PCSK9 Q152H , PCSK9 Q152D , and PCSK9 S386A and examined for the apoptosis markers caspase-3 and PUMA via real-time PCR.…”

“…The plasmids used in these studies included the bicistronic pIRES2-EGFP plasmids encoding V5-PCSK9 WT and its variants PCSK9 Q152S , PCSK9 Q152H , PCSK9 Q152D , and PCSK9 FS . VP WT and its variants VP G14R and VP G17V were cloned into pEGFP-N1 as described previously (21), and PCSK9 S386A was cloned into a pcDNA3.1 plasmid.…”

Loss-of-function PCSK9 mutants evade the unfolded protein response sensor GRP78 and fail to induce endoplasmic reticulum stress when retained

“…To assess whether the accumulation of misfolded proteins does indeed cause UPR activation in hepatocytes, HuH7 cells transfected with either PCSK9 WT or its ER-retention variant PCSK9 Q152H were compared with cells transfected with two VP variants, VP G14R and VP G17V , known to induce ER stress in N2a cells (20,21). Consistent with previous reports, our data demonstrate that ER retention of VP leads to UPR activation as determined by immunoblotting for GRP78 and IRE1␣ ( Fig.…”

“…A well-characterized ERSD occurring in liver results from a number of established mutations in ␣ 1 -antitrypsin Z that induce ER stress, liver cirrhosis, and hepatocellular carcinoma (35,36). Additional examples affecting other tissues include arginine vasopressin mutations (G14R and G17V) in familial neurohypophyseal diabetes insipidus (20,21,37), cystic fibrosis transmembrane conductance regulator ⌬F508 in cystic fibrosis (38), thyroglobulin mutations in congenital goiter and hyperthyroidism (39), and mutations in the Notch receptor that lead to cerebral autosomal-dominant arteriopathy and leukoencephalopathy (40).…”

“…A well-described form of ERSD occurs as a result of ER arginine vasopressin (VP) retention arising from mutations such as VP G14R and VP G17V . These naturally occurring mutations play a central role in the development of familial neurohypophyseal diabetes insipidus in a manner dependent on ER stress and subsequent UPR activation (20,21). The UPR signaling cascade consists of three major transducers located at the ER membrane that are activated upon dissociation of GRP78 from their intra-ER domains.…”

“…C and D, cell viability assays were carried out on transfected HK-2 and HuH7 cells using trypan blue stain and lactate dehydrogenase assays, respectively. E, a lactate dehydrogenase assay was also carried out on cells transfected with VP G17V , a mutant known to induce ER stress as a result of ER retention (21). F, freshly isolated mouse primary hepatocytes were transfected with PCSK9 variants PCSK9 Q152H , PCSK9 Q152D , and PCSK9 S386A and examined for the apoptosis markers caspase-3 and PUMA via real-time PCR.…”

“…The plasmids used in these studies included the bicistronic pIRES2-EGFP plasmids encoding V5-PCSK9 WT and its variants PCSK9 Q152S , PCSK9 Q152H , PCSK9 Q152D , and PCSK9 FS . VP WT and its variants VP G14R and VP G17V were cloned into pEGFP-N1 as described previously (21), and PCSK9 S386A was cloned into a pcDNA3.1 plasmid.…”

Loss-of-function PCSK9 mutants evade the unfolded protein response sensor GRP78 and fail to induce endoplasmic reticulum stress when retained

Two novel mutations in seven Czech and Slovak kindreds with familial neurohypophyseal diabetes insipidus—benefit of genetic testing

A novel AVP gene mutation in a Turkish family with neurohypophyseal diabetes insipidus