Mammalian TRIM67 Functions in Brain Development and Behavior

Boyer, Nicholas P.; Monkiewicz, Caroline; Menon, Shalini; Moy, Sheryl S.; Gupton, Stephanie L.

doi:10.1523/eneuro.0186-18.2018

Cited by 52 publications

(100 citation statements)

References 72 publications

(82 reference statements)

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“…No staining was observed on double KO mice brain slices (Figure 2B), indicating that the Abs in the CSF from patient 1 were only raised against TRIM9 and TRIM67. Immunostaining on Trim9 −/− single KO mouse brain found expression of TRIM67, and on Trim67 −/− mouse brain found expression of TRIM9 (Figure 2B); TRIM9 was widely expressed, notably in the hippocampus, and TRIM67 in the cerebellum, as previously described [6]. …”

Section: Resultssupporting

confidence: 82%

“…Immunostaining of Trim67 −/− mouse brain confirmed these observations. TRIM67 is abundantly expressed in the cerebellum of both mouse and human [6,11], and immunostaining with patient CSF herein showed a similar pattern.…”

Section: Discussionmentioning

confidence: 61%

“…Furthermore, in animal models, absence of TRIM9 causes excessive dendrite arborization, mislocalization and decreased dendritic density in adult born neurons of the dentate gyrus, leading to impairment of learning and memory [18]. TRIM67 interacts with TRIM9 and DCC and plays important role in brain development and behavior, including learning and memory and cognitive flexibility [6]. These two proteins seem therefore to play a major role in neuronal function, and we therefore investigated the pathogenicity of Abs on neurons.…”

Section: Discussionmentioning

confidence: 99%

“…Timed pregnant females were obtained by placing male and female mice together overnight; the following day was designated as E0.5 if the female had a vaginal plug. Trim9 −/− mice and Trim67 −/− mice have been previously described [5,6]. Trim9 −/− : Trim67 −/− mice, generated by crossing Trim9 −/− mice and Trim67 −/− mice, were viable and will be described in more detail below.…”

Section: Methodsmentioning

confidence: 99%

“…To confirm the target of the Abs, HEK 293 cells were transfected with pCS2- Trim9 (mouse) plasmid [8] or pCS2- Trim67 (mouse) plasmid [6] for transient overexpression. Fixed and permeabilized cells were then immunostained using patient CSF (1:100) and commercial mouse monoclonal anti-Myc antibody (ab9106, Abcam, Paris, France) and then they were revealed with appropriate fluorochrome-conjugated secondary antibodies (1:1500, A11013, and A11001, Thermofischer, Courtaboeuf, France).…”

Section: Methodsmentioning

confidence: 99%

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TRIM9 and TRIM67 Are New Targets in Paraneoplastic Cerebellar Degeneration

Gupton

Tanji

et al. 2018

Cerebellum

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Objective: To describe autoantibodies (Abs) against tripartite motif-containing (TRIM) protein 9 and 67 in two patients with paraneoplastic cerebellar degeneration (PCD) associated with lung adenocarcinoma. Methods: Abs were characterized using immunohistochemistry, Western blotting, cultures of murine cortical, and hippocampal neurons, immunoprecipitation, mass spectrometry, knockout mice for Trim9 and 67 and cell-based assay. Control samples included sera from 63 patients with small cell lung cancer without any paraneoplastic neurological syndrome, CSF from 100 patients with autoimmune encephalitis, and CSF from 165 patients with neurodegenerative diseases. Results: We found Abs targeting TRIM9 and TRIM67 at high concentration in the serum and the cerebrospinal fluid (CSF) of a 78-year-old woman and a 65-year-old man. Both developed subacute severe cerebellar ataxia. Brain magnetic resonance imaging found no abnormality and no cerebellar atrophy. Both had CSF inflammation with mild pleiocytosis and a few oligoclonal bands. We identified a pulmonary adenocarcinoma, confirming the paraneoplastic neurological syndrome in both patients. They received immunomodulatory and cancer treatments without improvement of cerebellar ataxia, even though both were in remission of their cancer (for more than 10 years in one patient). Anti-TRIM9 and anti-TRIM67 Abs were specific to these two patients. All control serum and CSF samples tested were negative for anti-TRIM9 and 67. Interpretation: Anti-TRIM9 and anti-TRIM67 Abs appeared to be specific biomarkers of PCD and should be added to the panel of antigens tested when this is suspected.

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Section: Resultssupporting

confidence: 82%

Section: Discussionmentioning

confidence: 61%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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TRIM9 and TRIM67 Are New Targets in Paraneoplastic Cerebellar Degeneration

Gupton

Tanji

et al. 2018

Cerebellum

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Detection of High‐Risk Paraneoplastic Antibodies against TRIM9 and TRIM67 Proteins

Bartley,

Ngo,

et al. 2023

Annals of Neurology

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Co‐occurring anti‐tripartite motif‐containing protein 9 and 67 autoantibodies (TRIM9/67‐IgG) have been reported in only a very few cases of paraneoplastic cerebellar syndrome. The value of these biomarkers and the most sensitive methods of TRIM9/67‐IgG detection are not known. We performed a retrospective, multi‐center study to evaluate the cerebrospinal fluid (CSF) and serum of candidate TRIM9/67‐IgG cases by tissue‐based immunofluorescence (TBIF), peptide phage display immunoprecipitation sequencing (PhIP‐Seq), overexpression cell‐based assay (CBA), and immunoblot. Cases in whom TRIM9/67‐IgG was detected by at least two assays were considered TRIM9/67‐IgG positive. Among these cases (N=13), CBA was the most sensitive (100%) and revealed that all cases had TRIM9 and TRIM67 autoantibodies. Of TRIM9/67‐IgG cases with available clinical history, a subacute cerebellar syndrome was the most common presentation (N = 7/10), followed by encephalitis (N = 3/10). Of these ten, 70% had comorbid cancer (7/10), 85% of whom (N = 6/7) had confirmed metastatic disease. All evaluable cancer biopsies expressed TRIM9 protein (N = 5/5), whose expression was elevated in the cancerous regions of the tissue in 4 of 5 cases. TRIM9/67‐IgG are rare but likely high‐risk paraneoplastic biomarkers for which CBA appears to be the most sensitive diagnostic assay.This article is protected by copyright. All rights reserved.

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Trim46 knockout impaired neuronal architecture and caused hypoactive behavior in rats

Guan,

Gao,

Sheng

et al. 2024

Developmental Dynamics

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BackgroundTripartite motif (TRIM46) is a relatively novel protein that belongs to tripartite motif family. TRIM46 organizes parallel microtubule arrays on the axons, which are important for neuronal polarity and axonal function. TRIM46 is highly expressed in the brain, but its biological function in adults has not yet been determined.ResultsTrim46 knockout (KO) rat line was established using CRISPR/cas9. Trim46 KO rats had smaller hippocampus sizes, fewer neuronal dendritic arbors and dendritic spines, and shorter and more distant axon initial segment. Furthermore, the protein interaction between endogenous TRIM46 and FK506 binding protein 5 (FKBP5) in brain tissues was determined; Trim46 KO increased hippocampal FKBP5 protein levels and decreased hippocampal protein kinase B (Akt) phosphorylation, gamma‐aminobutyric acid type A receptor subunit alpha1 (GABRA1) and glutamate ionotropic receptor NMDA type subunit 1 (NMDAR1) protein levels. Trim46 KO rats exhibited hypoactive behavioral changes such as reduced spontaneous activity, social interaction, sucrose preference, impaired prepulse inhibition (PPI), and short‐term reference memory.ConclusionsThese results demonstrate the significant impact of Trim46 KO on brain structure and behavioral function. This study revealed a novel potential association of TRIM46 with dendritic development and neuropsychiatric behavior, providing new insights into the role of TRIM46 in the brain.

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Mammalian TRIM67 Functions in Brain Development and Behavior

Cited by 52 publications

References 72 publications

TRIM9 and TRIM67 Are New Targets in Paraneoplastic Cerebellar Degeneration

TRIM9 and TRIM67 Are New Targets in Paraneoplastic Cerebellar Degeneration

Detection of High‐Risk Paraneoplastic Antibodies against TRIM9 and TRIM67 Proteins

Trim46 knockout impaired neuronal architecture and caused hypoactive behavior in rats

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