Novel insights into diabetes mellitus due to
            <i>
              <scp>DNAJC3</scp>
              ‐
            </i>
            defect: Evolution of neurological and endocrine phenotype in the pediatric age group

Özön, Z. Alev; Alikaşifoğlu, Ayfer; Kandemir, Nurgün; Aydın, Büşra; Gönç, E. Nazlı; Karaosmanoğlu, Beren; Celik, Nur Berna; Eroglu-Ertugrul, Nesibe Gevher; Taşkıran, Ekim Z.; Haliloğlu, Göknur; Oğuz, Kader Karlı; Kiper, Pelin Özlem Şimşek; Yalnızoğlu, Dilek; Ütine, Gülen Eda; Alikaşifoğlu, Mehmet

doi:10.1111/pedi.13098

Cited by 8 publications

(18 citation statements)

References 33 publications

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“…Of particular note most recently, two unrelated individuals presenting with a very similar phenotype to our siblings, that included hyperinsulinaemic hypoglycaemia, were found to be homozygous for different mutations at the same splice site c.393+2 T>G and c.393+2T>C (Ozon et al, 2020). These mutations are predicted to cause exon skipping and loss of protein function (Table 1).…”

Section: Genetic Findingsmentioning

confidence: 52%

Biallelic DNAJC3 variants in a neuroendocrine developmental disorder with insulin dysregulation

Ocansey

Pullen

Atkinson

et al. 2021

Clinical Dysmorphology

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DNAJC3, a co-chaperone of BiP, is a member of the heat shock protein family. These proteins are produced in the endoplasmic reticulum (ER) to counter cell stress resulting from healthy functional protein processing. Dysregulation of unfolded proteins within the ER is implicated as a mechanism of genetic disease. Examples include Marinesco-Sjogren and Wolcott-Rallison syndromes that share similar clinical features, manifesting neurodegenerative disease and endocrine dysfunction. Recently, loss of function mutations in DNAJC3 was associated with syndromic diabetes mellitus in three families. The full phenotype included neurodegeneration, ataxia, deafness, neuropathy, adolescent-onset diabetes mellitus, growth hormone deficiency and hypothyroidism. A subsequent report of two unrelated individuals extended the phenotype to include early-onset hyperinsulinaemic hypoglycaemia. Here, we describe two siblings that recapitulate this extended phenotype in association with a homozygous novel mutation in the final exon of DNAJC3 [c.1367_1370delAGAA (p.Lys456SerfsTer85)] resulting in protein elongation predicted to abrogate the functional J domain. This report confirms DNAJC3 as a cause of syndromic congenital hyperinsulinaemic hypoglycaemia. Currently, PanelApp only includes this gene on diabetes mellitus panels. We propose DNAJC3 should be promoted from a red to a green gene on a wider number of panels to improve the diagnosis of this rare condition.

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Section: Genetic Findingsmentioning

confidence: 52%

Biallelic DNAJC3 variants in a neuroendocrine developmental disorder with insulin dysregulation

Ocansey

Pullen

Atkinson

et al. 2021

Clinical Dysmorphology

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“…Finally, approximately 2 Mb downstream of the association signal on chromosome 12, the DnaJ heat shock protein family (Hsp40) member C3 ( DNAJC3 ) gene is located. This gene has been mainly implicated in the development of diabetes [ 37 , 38 ], but also neurodegeneration [ 37 ]. The pathomechanism of diabetes caused by DNAJC3 mutations further involves mitochondrial degeneration [ 39 ].…”

Section: Discussionmentioning

confidence: 99%

GWAS Hits for Bilateral Convergent Strabismus with Exophthalmos in Holstein Cattle Using Imputed Sequence Level Genotypes

Bögeholz

Falker‐Gieske

Guélat

et al. 2021

Genes

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Bilateral convergent strabismus with exophthalmos (BCSE) is a malformation of the eyes and is recognized as a mild but progressive disorder that affects cattle in the first two years of life. This most likely inherited disorder is rarely described in cattle resembling autosomal dominantly inherited forms of human progressive external ophthalmoplegia (PEO). In German Braunvieh cattle, two linked genome regions were found that could be responsible for the development and/or progression of BCSE. The goal of this study was to phenotypically characterize BCSE in Holstein cattle from Germany and Switzerland as well as to identify associated genome regions by GWAS. The clinicopathological phenotype of 52 BCSE-affected Holstein cattle was in accordance with the phenotype described in German Braunvieh cattle, but in addition, signs of degeneration and cellular infiltration in the eye muscles were found. By using imputed sequence level genotype data, three genome-wide significant GWAS hits were revealed on different chromosomes that were not detected by initial GWAS based on high density SNP array data highlighting the usefulness of this approach for mapping studies. The associated genome regions include the ABCC4 gene as well as markers adjacent to the NCOR2 and DNAJC3 genes all illustrating possible functional candidate genes. Our results challenge a monogenic mode of inheritance and indicate a more complex inheritance of BCSE in Holstein cattle. Furthermore, in comparison to previous results from German Braunvieh cattle, it illustrates an obvious genetic heterogeneity causing BSCE in cattle. Subsequent whole genome sequencing (WGS)-based analyses might elucidate pathogenic variants in the future.

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“…Mutant variants of BiP interaction partners are associated with the manifestation of neurological diseases [ 275 , 276 , 277 , 278 , 279 , 280 , 281 , 282 , 283 , 284 , 285 , 286 , 287 , 288 , 289 , 290 , 291 , 292 , 293 , 294 , 295 , 296 , 297 , 298 , 299 , 300 , 301 , 302 , 303 , 304 , 305 ]. In 2005, recessive SIL1 mutations were linked to the phenotypical manifestation of Marinesco–Sjögren syndrome (MSS; MIM: 248800) ( Figure 8 ), a rare autosomal recessively inherited multisystemic disorder characterized by a vacuolar myopathy, congenital or infantile manifesting cataracts and cerebellar atrophy leading to ataxia ( Figure 8 b) [ 276 , 277 ].…”

Section: Diseases That Are Related To Allosteric Effectors Of the Sec61 Channelmentioning

confidence: 99%

“…In vivo studies utilizing the “woozy” mouse model revealed that decrease of ERj6 ameliorates ER stress and neurodegeneration in these animals suggesting that alterations in the nucleotide exchange reaction of BiP cause ER stress and neurodegeneration in Sil1-deficient neurons [ 278 , 279 ]. In 2014, recessive DNAJC3 mutations were linked to Diabetes mellitus complicated by multisystemic neurodegeneration including ataxia, upper-motor-neuron damage, peripheral neuropathy, sensorineural hearing loss, and cerebral atrophy [ 261 ] (MIM: 616192) and a further clinical and molecular genetic study confirmed the phenotype associated with recessive loss of function mutations within DNAJC3 [ 292 ]. Although precise molecular data unravelling the underlying pathomechanisms are still scarce a recent study points at BIM- and PUMA-dependent activation of the mitochondrial pathway of apoptosis [ 292 ].…”

Section: Diseases That Are Related To Allosteric Effectors Of the Sec61 Channelmentioning

confidence: 99%

Complexity and Specificity of Sec61-Channelopathies: Human Diseases Affecting Gating of the Sec61 Complex

Sicking

Lang

Bochen

et al. 2021

Cells

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The rough endoplasmic reticulum (ER) of nucleated human cells has crucial functions in protein biogenesis, calcium (Ca2+) homeostasis, and signal transduction. Among the roughly one hundred components, which are involved in protein import and protein folding or assembly, two components stand out: The Sec61 complex and BiP. The Sec61 complex in the ER membrane represents the major entry point for precursor polypeptides into the membrane or lumen of the ER and provides a conduit for Ca2+ ions from the ER lumen to the cytosol. The second component, the Hsp70-type molecular chaperone immunoglobulin heavy chain binding protein, short BiP, plays central roles in protein folding and assembly (hence its name), protein import, cellular Ca2+ homeostasis, and various intracellular signal transduction pathways. For the purpose of this review, we focus on these two components, their relevant allosteric effectors and on the question of how their respective functional cycles are linked in order to reconcile the apparently contradictory features of the ER membrane, selective permeability for precursor polypeptides, and impermeability for Ca2+. The key issues are that the Sec61 complex exists in two conformations: An open and a closed state that are in a dynamic equilibrium with each other, and that BiP contributes to its gating in both directions in cooperation with different co-chaperones. While the open Sec61 complex forms an aqueous polypeptide-conducting- and transiently Ca2+-permeable channel, the closed complex is impermeable even to Ca2+. Therefore, we discuss the human hereditary and tumor diseases that are linked to Sec61 channel gating, termed Sec61-channelopathies, as disturbances of selective polypeptide-impermeability and/or aberrant Ca2+-permeability.

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Novel insights into diabetes mellitus due to DNAJC3 ‐ defect: Evolution of neurological and endocrine phenotype in the pediatric age group

Cited by 8 publications

References 33 publications

Biallelic DNAJC3 variants in a neuroendocrine developmental disorder with insulin dysregulation

Biallelic DNAJC3 variants in a neuroendocrine developmental disorder with insulin dysregulation

GWAS Hits for Bilateral Convergent Strabismus with Exophthalmos in Holstein Cattle Using Imputed Sequence Level Genotypes

Complexity and Specificity of Sec61-Channelopathies: Human Diseases Affecting Gating of the Sec61 Complex

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