Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation

Alyssa N. Coyne; Shizuka B. Yamada; Bhavani Bagevalu Siddegowda; Patricia S. Estes; Benjamin L. Zaepfel; Jeffrey S. Johannesmeyer; Donovan B. Lockwood; Linh T. Pham; Michael P. Hart; Joel A. Cassel; Brian Freibaum; Ashley V. Boehringer; J. Paul Taylor; Allen B. Reitz; Aaron D. Gitler; Daniela C. Zarnescu

doi:10.1093/hmg/ddv389

Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation

Alyssa N. Coyne
, Shizuka B. Yamada
, Bhavani Bagevalu Siddegowda
, Patricia S. Estes
, Benjamin L. Zaepfel
, Jeffrey S. Johannesmeyer
, Donovan B. Lockwood
, Linh T. Pham
, Michael P. Hart
, Joel A. Cassel
, Brian Freibaum
, Ashley V. Boehringer
, J. Paul Taylor
, Allen B. Reitz
, Aaron D. Gitler
, Daniela C. Zarnescu

Research output: Contribution to journal › Article › peer-review

73 Citations (SciVal)

Abstract

RNA dysregulation is a newly recognized disease mechanism in amyotrophic lateral sclerosis (ALS). Here we identify Drosophila fragile X mental retardation protein (dFMRP) as a robust genetic modifier of TDP-43-dependent toxicity in a Drosophila model of ALS.We find that dFMRP overexpression (dFMRP OE) mitigates TDP-43 dependent locomotor defects and reduced lifespan in Drosophila. TDP-43 and FMRP form a complex in flies and human cells. In motor neurons, TDP-43 expression increases the association of dFMRP with stress granules and colocalizes with polyA binding protein in a variant-dependent manner. Furthermore, dFMRP dosage modulates TDP-43 solubility and molecular mobility with overexpression of dFMRP resulting in a significant reduction of TDP-43 in the aggregate fraction. Polysome fractionation experiments indicate that dFMRP OE also relieves the translation inhibition of futsch mRNA, a TDP-43 target mRNA, which regulates neuromuscular synapse architecture. Restoration of futsch translation by dFMRP OE mitigates Futsch-dependent morphological phenotypes at the neuromuscular junction including synaptic size and presence of satellite boutons. Our data suggest a model whereby dFMRP is neuroprotective by remodeling TDP-43 containing RNA granules, reducing aggregation and restoring the translation of specific mRNAs in motor neurons.

Original language	English (US)
Pages (from-to)	6886-6898
Number of pages	13
Journal	Human molecular genetics
Volume	24
Issue number	24
DOIs	https://doi.org/10.1093/hmg/ddv389
State	Published - 2015

All Science Journal Classification (ASJC) codes

Molecular Biology
Genetics
Genetics(clinical)

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10.1093/hmg/ddv389

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Coyne, A. N., Yamada, S. B., Siddegowda, B. B., Estes, P. S., Zaepfel, B. L., Johannesmeyer, J. S., Lockwood, D. B., Pham, L. T., Hart, M. P., Cassel, J. A., Freibaum, B., Boehringer, A. V., Paul Taylor, J., Reitz, A. B., Gitler, A. D., & Zarnescu, D. C. (2015). Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation. Human molecular genetics, 24(24), 6886-6898. https://doi.org/10.1093/hmg/ddv389

@article{ccc7f9e322b04bcfa707469d05f081d4,

title = "Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation",

abstract = "RNA dysregulation is a newly recognized disease mechanism in amyotrophic lateral sclerosis (ALS). Here we identify Drosophila fragile X mental retardation protein (dFMRP) as a robust genetic modifier of TDP-43-dependent toxicity in a Drosophila model of ALS.We find that dFMRP overexpression (dFMRP OE) mitigates TDP-43 dependent locomotor defects and reduced lifespan in Drosophila. TDP-43 and FMRP form a complex in flies and human cells. In motor neurons, TDP-43 expression increases the association of dFMRP with stress granules and colocalizes with polyA binding protein in a variant-dependent manner. Furthermore, dFMRP dosage modulates TDP-43 solubility and molecular mobility with overexpression of dFMRP resulting in a significant reduction of TDP-43 in the aggregate fraction. Polysome fractionation experiments indicate that dFMRP OE also relieves the translation inhibition of futsch mRNA, a TDP-43 target mRNA, which regulates neuromuscular synapse architecture. Restoration of futsch translation by dFMRP OE mitigates Futsch-dependent morphological phenotypes at the neuromuscular junction including synaptic size and presence of satellite boutons. Our data suggest a model whereby dFMRP is neuroprotective by remodeling TDP-43 containing RNA granules, reducing aggregation and restoring the translation of specific mRNAs in motor neurons.",

author = "Coyne, \{Alyssa N.\} and Yamada, \{Shizuka B.\} and Siddegowda, \{Bhavani Bagevalu\} and Estes, \{Patricia S.\} and Zaepfel, \{Benjamin L.\} and Johannesmeyer, \{Jeffrey S.\} and Lockwood, \{Donovan B.\} and Pham, \{Linh T.\} and Hart, \{Michael P.\} and Cassel, \{Joel A.\} and Brian Freibaum and Boehringer, \{Ashley V.\} and \{Paul Taylor\}, J. and Reitz, \{Allen B.\} and Gitler, \{Aaron D.\} and Zarnescu, \{Daniela C.\}",

note = "Publisher Copyright: {\textcopyright} The Author 2015. Published by Oxford University Press.",

year = "2015",

doi = "10.1093/hmg/ddv389",

language = "English (US)",

volume = "24",

pages = "6886--6898",

journal = "Human molecular genetics",

issn = "0964-6906",

publisher = "Oxford University Press",

number = "24",

}

Coyne, AN, Yamada, SB, Siddegowda, BB, Estes, PS, Zaepfel, BL, Johannesmeyer, JS, Lockwood, DB, Pham, LT, Hart, MP, Cassel, JA, Freibaum, B, Boehringer, AV, Paul Taylor, J, Reitz, AB, Gitler, AD & Zarnescu, DC 2015, 'Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation', Human molecular genetics, vol. 24, no. 24, pp. 6886-6898. https://doi.org/10.1093/hmg/ddv389

TY - JOUR

T1 - Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation

AU - Coyne, Alyssa N.

AU - Yamada, Shizuka B.

AU - Siddegowda, Bhavani Bagevalu

AU - Estes, Patricia S.

AU - Zaepfel, Benjamin L.

AU - Johannesmeyer, Jeffrey S.

AU - Lockwood, Donovan B.

AU - Pham, Linh T.

AU - Hart, Michael P.

AU - Cassel, Joel A.

AU - Freibaum, Brian

AU - Boehringer, Ashley V.

AU - Paul Taylor, J.

AU - Reitz, Allen B.

AU - Gitler, Aaron D.

AU - Zarnescu, Daniela C.

PY - 2015

Y1 - 2015

N2 - RNA dysregulation is a newly recognized disease mechanism in amyotrophic lateral sclerosis (ALS). Here we identify Drosophila fragile X mental retardation protein (dFMRP) as a robust genetic modifier of TDP-43-dependent toxicity in a Drosophila model of ALS.We find that dFMRP overexpression (dFMRP OE) mitigates TDP-43 dependent locomotor defects and reduced lifespan in Drosophila. TDP-43 and FMRP form a complex in flies and human cells. In motor neurons, TDP-43 expression increases the association of dFMRP with stress granules and colocalizes with polyA binding protein in a variant-dependent manner. Furthermore, dFMRP dosage modulates TDP-43 solubility and molecular mobility with overexpression of dFMRP resulting in a significant reduction of TDP-43 in the aggregate fraction. Polysome fractionation experiments indicate that dFMRP OE also relieves the translation inhibition of futsch mRNA, a TDP-43 target mRNA, which regulates neuromuscular synapse architecture. Restoration of futsch translation by dFMRP OE mitigates Futsch-dependent morphological phenotypes at the neuromuscular junction including synaptic size and presence of satellite boutons. Our data suggest a model whereby dFMRP is neuroprotective by remodeling TDP-43 containing RNA granules, reducing aggregation and restoring the translation of specific mRNAs in motor neurons.

AB - RNA dysregulation is a newly recognized disease mechanism in amyotrophic lateral sclerosis (ALS). Here we identify Drosophila fragile X mental retardation protein (dFMRP) as a robust genetic modifier of TDP-43-dependent toxicity in a Drosophila model of ALS.We find that dFMRP overexpression (dFMRP OE) mitigates TDP-43 dependent locomotor defects and reduced lifespan in Drosophila. TDP-43 and FMRP form a complex in flies and human cells. In motor neurons, TDP-43 expression increases the association of dFMRP with stress granules and colocalizes with polyA binding protein in a variant-dependent manner. Furthermore, dFMRP dosage modulates TDP-43 solubility and molecular mobility with overexpression of dFMRP resulting in a significant reduction of TDP-43 in the aggregate fraction. Polysome fractionation experiments indicate that dFMRP OE also relieves the translation inhibition of futsch mRNA, a TDP-43 target mRNA, which regulates neuromuscular synapse architecture. Restoration of futsch translation by dFMRP OE mitigates Futsch-dependent morphological phenotypes at the neuromuscular junction including synaptic size and presence of satellite boutons. Our data suggest a model whereby dFMRP is neuroprotective by remodeling TDP-43 containing RNA granules, reducing aggregation and restoring the translation of specific mRNAs in motor neurons.

UR - https://www.scopus.com/pages/publications/84952862498

UR - https://www.scopus.com/pages/publications/84952862498#tab=citedBy

U2 - 10.1093/hmg/ddv389

DO - 10.1093/hmg/ddv389

M3 - Article

C2 - 26385636

AN - SCOPUS:84952862498

SN - 0964-6906

VL - 24

SP - 6886

EP - 6898

JO - Human molecular genetics

JF - Human molecular genetics

IS - 24

ER -

Fragile X protein mitigates TDP-43 toxicity by remodeling RNA granules and restoring translation

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