Deficiencies in vesicular transport mediated by TRAPPC4 are associated with severe syndromic intellectual disability

Bergen, Nicole J Van; Guo, Yiran; Al-Deri, Noraldin; Lipatova, Zhanna; Stanga, Daniela; Zhao, Sarah F; Murtazina, Rakhilya; Gyurkovska, Valeriya; Pehlivan, Davut; Mitani, Tadahiro; Gezdirici, Alper; Antony, Jayne; Collins, Felicity; Willis, Mary; Akdemir, Zeynep H. Coban; Liu, Pengfei; Punetha, Jaya; Hunter, Jill V.; Jhangiani, Shalini N.; Fatih, Jawid M.; Rosenfeld, Jill A.; Posey, Jennifer E.; Gibbs, Richard A.; Karaca, Ender; Massey, Sean; Ranasinghe, Thisara G; Sleiman, Patrick; Troedson, Chris; Lupski, James R.; Sacher, Michael; Segev, Nava; Hákonarson, Hákon; Christodoulou, John

doi:10.1093/brain/awz374

Cited by 34 publications

(29 citation statements)

References 73 publications

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“…Therefore, further studies are needed to determine whether mTRAPP-II is a bona fide GEF for rab11. The function of mTRAPP in mammals is largely unknown, but genetic mutations disabling several mTRAPP subunits have been linked to ID with brain malformations similar to trappc9linked ID (20)(21)(22)(23)(24)(25). The lack of genetically modified mammals deficient for mTRAPP subunit(s) restricts us from exploring pathogenic mechanisms and therapeutic strategies for these diseases.…”

Section: Introductionmentioning

confidence: 99%

Trappc9 deficiency in mice impairs learning and memory by causing imbalance of dopamine D1 and D2 neurons

Weng

Chhetri

et al. 2020

Sci. Adv.

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Genetic mutations in the gene encoding transport protein particle complex 9 (trappc9), a subunit of TRAPP that acts as a guanine nucleotide exchange factor for rab proteins, cause intellectual disability with brain structural malformations by elusive mechanisms. Here, we report that trappc9-deficient mice exhibit a broad range of behavioral deficits and postnatal delay in growth of the brain. Contrary to volume decline of various brain structures, the striatum of trappc9 null mice was enlarged. An imbalance existed between dopamine D1 and D2 receptor containing neurons in the brain of trappc9-deficient mice; pharmacological manipulation of dopamine receptors improved performances of trappc9 null mice to levels of wild-type mice on cognitive tasks. Loss of trappc9 compromised the activation of rab11 in the brain and resulted in retardation of endocytic receptor recycling in neurons. Our study elicits a pathogenic mechanism and a potential treatment for trappc9-linked disorders including intellectual disability.

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Section: Introductionmentioning

confidence: 99%

Trappc9 deficiency in mice impairs learning and memory by causing imbalance of dopamine D1 and D2 neurons

Weng

Chhetri

et al. 2020

Sci. Adv.

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“…Highlighting the critical roles of the TRAPP complexes in myriad cellular processes has been the discovery of a spectrum of human diseases caused by mutations in different TRAPP subunits, collectively known as TRAPPopathies 5,7,[28][29][30][31][32][33][34][35] . Disorders associated with these mutations include the developmental disorder spondyloepiphyseal dysplasia tarda (SEDT), neurodevelopmental delay, microcephaly, epilepsy, and severe intellectual disability.…”

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confidence: 99%

The substrate specificity of the human TRAPPII complex’s Rab-guanine nucleotide exchange factor activity

et al. 2020

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The TRAnsport Protein Particle (TRAPP) complexes act as Guanine nucleotide exchange factors (GEFs) for Rab GTPases, which are master regulators of membrane trafficking in eukaryotic cells. In metazoans, there are two large multi-protein TRAPP complexes: TRAPPII and TRAPPIII, with the TRAPPII complex able to activate both Rab1 and Rab11. Here we present detailed biochemical characterisation of Rab-GEF specificity of the human TRAPPII complex, and molecular insight into Rab binding. GEF assays of the TRAPPII complex against a panel of 20 different Rab GTPases revealed GEF activity on Rab43 and Rab19. Electron microscopy and chemical cross-linking revealed the architecture of mammalian TRAPPII. Hydrogen deuterium exchange MS showed that Rab1, Rab11 and Rab43 share a conserved binding interface. Clinical mutations in Rab11, and phosphomimics of Rab43, showed decreased TRAPPII GEF mediated exchange. Finally, we designed a Rab11 mutation that maintained TRAPPII-mediated GEF activity while decreasing activity of the Rab11-GEF SH3BP5, providing a tool to dissect Rab11 signalling. Overall, our results provide insight into the GTPase specificity of TRAPPII, and how clinical mutations disrupt this regulation.

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“…TPC6A is a member of the TRAPP family. The family proteins have been shown to be associated with neural diseases such as AD [ 78 , 79 ].…”

Section: Wwox In Alzheimer’s Diseasementioning

confidence: 99%

WWOX and Its Binding Proteins in Neurodegeneration

Hsu

Lee

Sun

et al. 2021

Cells

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WW domain-containing oxidoreductase (WWOX) is known as one of the risk factors for Alzheimer’s disease (AD), a neurodegenerative disease. WWOX binds Tau via its C-terminal SDR domain and interacts with Tau phosphorylating enzymes ERK, JNK, and GSK-3β, and thereby limits AD progression. Loss of WWOX in newborns leads to severe neural diseases and early death. Gradual loss of WWOX protein in the hippocampus and cortex starting from middle age may slowly induce aggregation of a protein cascade that ultimately causes accumulation of extracellular amyloid beta plaques and intracellular tau tangles, along with reduction in inhibitory GABAergic interneurons, in AD patients over 70 years old. Age-related increases in pS14-WWOX accumulation in the brain promotes neuronal degeneration. Suppression of Ser14 phosphorylation by a small peptide Zfra leads to enhanced protein degradation, reduction in NF-κB-mediated inflammation, and restoration of memory loss in triple transgenic mice for AD. Intriguingly, tumor suppressors p53 and WWOX may counteract each other in vivo, which leads to upregulation of AD-related protein aggregation in the brain and lung. WWOX has numerous binding proteins. We reported that the stronger the binding between WWOX and its partners, the better the suppression of cancer growth and reduction in inflammation. In this regard, the stronger complex formation between WWOX and partners may provide a better blockade of AD progression. In this review, we describe whether and how WWOX and partner proteins control inflammatory response and protein aggregation and thereby limit AD progression.

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Deficiencies in vesicular transport mediated by TRAPPC4 are associated with severe syndromic intellectual disability

Cited by 34 publications

References 73 publications

Trappc9 deficiency in mice impairs learning and memory by causing imbalance of dopamine D1 and D2 neurons

Trappc9 deficiency in mice impairs learning and memory by causing imbalance of dopamine D1 and D2 neurons

The substrate specificity of the human TRAPPII complex’s Rab-guanine nucleotide exchange factor activity

WWOX and Its Binding Proteins in Neurodegeneration

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