Molecular switch of the dendrite-to-spine transport of TDP-43/FMRP-bound neuronal mRNAs and its impairment in ASD

Pritha Majumder; Biswanath Chatterjee; Khadiza Akter; Asmar Ahsan; Su Jie Tan; Chi-Chen Huang; Jen-Fei Chu; Che-Kun James Shen

doi:10.1186/s11658-024-00684-5

Molecular switch of the dendrite-to-spine transport of TDP-43/FMRP-bound neuronal mRNAs and its impairment in ASD

Cell Mol Biol Lett. 2025 Jan 15;30(1):6. doi: 10.1186/s11658-024-00684-5.

Authors

Pritha Majumder^{1

2}, Biswanath Chatterjee³, Khadiza Akter³, Asmar Ahsan³, Su Jie Tan⁴, Chi-Chen Huang³, Jen-Fei Chu⁵, Che-Kun James Shen^{6

7}

Affiliations

¹ PhD Program in Medical Neuroscience, Taipei Medical University, Taipei, Taiwan (R.O.C.). [email protected].
² Institute of Molecular Medicine, College of Medicine, National Chen Kung University, Tainan, Taiwan (R.O.C.). [email protected].
³ PhD Program in Medical Neuroscience, Taipei Medical University, Taipei, Taiwan (R.O.C.).
⁴ Institute of Molecular Medicine, College of Medicine, National Chen Kung University, Tainan, Taiwan (R.O.C.).
⁵ PhD Program in Medical Neuroscience, Taipei Medical University, Taipei, Taiwan (R.O.C.). [email protected].
⁶ PhD Program in Medical Neuroscience, Taipei Medical University, Taipei, Taiwan (R.O.C.). [email protected].
⁷ Institute of Molecular Biology, Academia Sinica, Nangang, Taipei, 115, Taiwan (R.O.C.). [email protected].

PMID: 39815169
DOI: 10.1186/s11658-024-00684-5

Abstract

Background: Regulation of messenger RNA (mRNA) transport and translation in neurons is essential for dendritic plasticity and learning/memory development. The trafficking of mRNAs along the hippocampal neuron dendrites remains translationally silent until they are selectively transported into the spines upon glutamate-induced receptor activation. However, the molecular mechanism(s) behind the spine entry of dendritic mRNAs under metabotropic glutamate receptor (mGluR)-mediated neuroactivation and long-term depression (LTD) as well as the fate of these mRNAs inside the spines are still elusive.

Method: Different molecular and imaging techniques, e.g., immunoprecipitation (IP), RNA-IP, Immunofluorescence (IF)/fluorescence in situ hybridization (FISH), live cell imaging, live cell tracking of RNA using beacon, and mouse model study are used to elucidate a novel mechanism regulating dendritic spine transport of mRNAs in mammalian neurons.

Results: We demonstrate here that brief mGluR1 activation-mediated dephosphorylation of pFMRP (S499) results in the dissociation of FMRP from TDP-43 and handover of TDP-43/Rac1 mRNA complex from the dendritic transport track on microtubules to myosin V track on the spine actin filaments. Rac1 mRNA thus enters the spines for translational reactivation and increases the mature spine density. In contrast, during mGluR1-mediated neuronal LTD, FMRP (S499) remains phosphorylated and the TDP-43/Rac1 mRNA complex, being associated with kinesin 1-FMRP/cortactin/drebrin, enters the spines owing to Ca²⁺-dependent microtubule invasion into spines, but without translational reactivation. In a VPA-ASD mouse model, this regulation become anomalous.

Conclusions: This study, for the first time, highlights the importance of posttranslational modification of RBPs, such as the neurodevelopmental disease-related protein FMRP, as the molecular switch regulating the dendrite-to-spine transport of specific mRNAs under mGluR1-mediated neurotransmissions. The misregulation of this switch could contribute to the pathogenesis of FMRP-related neurodisorders including the autism spectrum disorder (ASD). It also could indicate a molecular connection between ASD and neurodegenerative disease-related protein TDP-43 and opens up a new perspective of research to elucidate TDP-43 proteinopathy among patients with ASD.

Keywords: DHPG; High-resolution imaging; Immunofluorescence staining; Kinase; Live cell imaging; Long-term depression (LTD); Phosphatase; Posttranslational modification; Potentiation; RNA binding protein (RBP); TDP-43; Translation status; mRNP granule; pFMRP (S499).

Abstract

Grants and funding