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Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
by Walden, Michael , Meyer-Schwesinger, Catherine , Damme, Markus , Janiesch, Philipp Christoph , Sachs, Wiebke , Reichelt, Julia , Reinicke, Anna T. , Laban, Karoline , Duncan, Kent E. , Saftig, Paul , Rinschen, Markus M. , Morellini, Fabio , Kraus, Vanessa , Sachs, Marlies , Schweizer, Michaela
in Acceleration / Accumulation / Animal models / Animals / Biodegradation / Biological Sciences / Degeneration / Depletion / Disease Models, Animal / Endoplasmic reticulum / Female / Homeostasis / Hydrolase / Male / Medical Sciences / Mice / Mice, Transgenic / Neurodegeneration / Neurodegenerative Diseases - metabolism / Neurodegenerative Diseases - physiopathology / Neurons / Neurons - metabolism / Phenotypes / PNAS Plus / Proteasome Endopeptidase Complex - metabolism / Proteasomes / Protein Biosynthesis / Protein gene product 9.5 / Protein synthesis / Protein turnover / Proteins / Rapamycin / Rodents / Sensorimotor system / Substrates / TOR Serine-Threonine Kinases - metabolism / Transgenic mice / Ubiquitin / Ubiquitin Thiolesterase - deficiency / Ubiquitin Thiolesterase - genetics / Ubiquitin Thiolesterase - physiology
2019
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Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
by Walden, Michael , Meyer-Schwesinger, Catherine , Damme, Markus , Janiesch, Philipp Christoph , Sachs, Wiebke , Reichelt, Julia , Reinicke, Anna T. , Laban, Karoline , Duncan, Kent E. , Saftig, Paul , Rinschen, Markus M. , Morellini, Fabio , Kraus, Vanessa , Sachs, Marlies , Schweizer, Michaela
in Acceleration / Accumulation / Animal models / Animals / Biodegradation / Biological Sciences / Degeneration / Depletion / Disease Models, Animal / Endoplasmic reticulum / Female / Homeostasis / Hydrolase / Male / Medical Sciences / Mice / Mice, Transgenic / Neurodegeneration / Neurodegenerative Diseases - metabolism / Neurodegenerative Diseases - physiopathology / Neurons / Neurons - metabolism / Phenotypes / PNAS Plus / Proteasome Endopeptidase Complex - metabolism / Proteasomes / Protein Biosynthesis / Protein gene product 9.5 / Protein synthesis / Protein turnover / Proteins / Rapamycin / Rodents / Sensorimotor system / Substrates / TOR Serine-Threonine Kinases - metabolism / Transgenic mice / Ubiquitin / Ubiquitin Thiolesterase - deficiency / Ubiquitin Thiolesterase - genetics / Ubiquitin Thiolesterase - physiology
2019
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Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
by Walden, Michael , Meyer-Schwesinger, Catherine , Damme, Markus , Janiesch, Philipp Christoph , Sachs, Wiebke , Reichelt, Julia , Reinicke, Anna T. , Laban, Karoline , Duncan, Kent E. , Saftig, Paul , Rinschen, Markus M. , Morellini, Fabio , Kraus, Vanessa , Sachs, Marlies , Schweizer, Michaela
in Acceleration / Accumulation / Animal models / Animals / Biodegradation / Biological Sciences / Degeneration / Depletion / Disease Models, Animal / Endoplasmic reticulum / Female / Homeostasis / Hydrolase / Male / Medical Sciences / Mice / Mice, Transgenic / Neurodegeneration / Neurodegenerative Diseases - metabolism / Neurodegenerative Diseases - physiopathology / Neurons / Neurons - metabolism / Phenotypes / PNAS Plus / Proteasome Endopeptidase Complex - metabolism / Proteasomes / Protein Biosynthesis / Protein gene product 9.5 / Protein synthesis / Protein turnover / Proteins / Rapamycin / Rodents / Sensorimotor system / Substrates / TOR Serine-Threonine Kinases - metabolism / Transgenic mice / Ubiquitin / Ubiquitin Thiolesterase - deficiency / Ubiquitin Thiolesterase - genetics / Ubiquitin Thiolesterase - physiology
2019

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Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks
Journal Article

Ubiquitin C-terminal hydrolase L1 (UCH-L1) loss causes neurodegeneration by altering protein turnover in the first postnatal weeks

Walden, Michael,
Meyer-Schwesinger, Catherine,
Damme, Markus,
Janiesch, Philipp Christoph,
Sachs, Wiebke,
Reichelt, Julia,
Reinicke, Anna T.,
Laban, Karoline,
Duncan, Kent E.,
Saftig, Paul,
Rinschen, Markus M.,
Morellini, Fabio,
Kraus, Vanessa,
Sachs, Marlies,
Schweizer, Michaela
2019
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Overview
Ubiquitin C-terminal hydrolase L1 (UCH-L1) is one of the most abundant and enigmatic enzymes of the CNS. Based on existing UCH-L1 knockout models, UCH-L1 is thought to be required for the maintenance of axonal integrity, but not for neuronal development despite its high expression in neurons. Several lines of evidence suggest a role for UCH-L1 in mUB homeostasis, although the specific in vivo substrate remains elusive. Since the precise mechanisms underlying UCH-L1–deficient neurodegeneration remain unclear, we generated a transgenic mouse model of UCH-L1 deficiency. By performing biochemical and behavioral analyses we can show that UCH-L1 deficiency causes an acceleration of sensorimotor reflex development in the first postnatal week followed by a degeneration of motor function starting at periadolescence in the setting of normal cerebral mUB levels. In the first postnatal weeks, neuronal protein synthesis and proteasomal protein degradation are enhanced, with endoplasmic reticulum stress, and energy depletion, leading to proteasomal impairment and an accumulation of nondegraded ubiquitinated protein. Increased protein turnover is associated with enhanced mTORC1 activity restricted to the postnatal period in UCH-L1–deficient brains. Inhibition of mTORC1 with rapamycin decreases protein synthesis and ubiquitin accumulation in UCH-L1–deficient neurons. Strikingly, rapamycin treatment in the first 8 postnatal days ameliorates the neurological phenotype of UCH-L1–deficient mice up to 16 weeks, suggesting that early control of protein homeostasis is imperative for long-term neuronal survival. In summary, we identified a critical presymptomatic period during which UCH-L1–dependent enhanced protein synthesis results in neuronal strain and progressive loss of neuronal function.
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Publisher
National Academy of Sciences
Subject

Acceleration

/ Accumulation

/ Animal models

/ Animals

/ Biodegradation

/ Biological Sciences

/ Degeneration

/ Depletion

/ Disease Models, Animal

/ Endoplasmic reticulum

/ Female

/ Homeostasis

/ Hydrolase

/ Male

/ Medical Sciences

/ Mice

/ Mice, Transgenic

/ Neurodegeneration

/ Neurodegenerative Diseases - metabolism

/ Neurodegenerative Diseases - physiopathology

/ Neurons

/ Neurons - metabolism

/ Phenotypes

/ PNAS Plus

/ Proteasome Endopeptidase Complex - metabolism

/ Proteasomes

/ Protein Biosynthesis

/ Protein gene product 9.5

/ Protein synthesis

/ Protein turnover

/ Proteins

/ Rapamycin

/ Rodents

/ Sensorimotor system

/ Substrates

/ TOR Serine-Threonine Kinases - metabolism

/ Transgenic mice

/ Ubiquitin

/ Ubiquitin Thiolesterase - deficiency

/ Ubiquitin Thiolesterase - genetics

/ Ubiquitin Thiolesterase - physiology

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