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The Parkinson-associated protein PINK1 interacts with Beclin1 and promotes autophagy
by
Michiorri, S
, Giarda, E
, Nerini-Molteni, S
, Russo, M A
, Arena, G
, Torosantucci, L
, Dallapiccola, B
, Lombardi, F
, Marongiu, R
, Casari, G
, Vago, R
, Cassina, L
, Valente, E M
, Romano, F
, Sale, P
, Gelmetti, V
in
631/378/1689/1718
/ 631/80/82/39/2348
/ 631/80/86
/ 692/420
/ Apoptosis
/ Apoptosis Regulatory Proteins - analysis
/ Apoptosis Regulatory Proteins - metabolism
/ Autophagy
/ Beclin-1
/ Biochemistry
/ Biomedical and Life Sciences
/ Cell Biology
/ Cell Cycle Analysis
/ Cell death
/ Cell division
/ Cell Line, Tumor
/ Disease
/ HeLa Cells
/ Humans
/ Kinases
/ Life Sciences
/ Membrane Proteins - analysis
/ Membrane Proteins - metabolism
/ Mitochondria
/ Mitochondria - chemistry
/ Mitochondria - ultrastructure
/ Morphology
/ Mutation
/ Neurodegeneration
/ original-paper
/ Parkinson's disease
/ Protein Kinases - analysis
/ Protein Kinases - genetics
/ Protein Kinases - metabolism
/ Proteins
/ Quality control
/ Sequence Deletion
/ Stem Cells
/ Two-Hybrid System Techniques
2010
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The Parkinson-associated protein PINK1 interacts with Beclin1 and promotes autophagy
by
Michiorri, S
, Giarda, E
, Nerini-Molteni, S
, Russo, M A
, Arena, G
, Torosantucci, L
, Dallapiccola, B
, Lombardi, F
, Marongiu, R
, Casari, G
, Vago, R
, Cassina, L
, Valente, E M
, Romano, F
, Sale, P
, Gelmetti, V
in
631/378/1689/1718
/ 631/80/82/39/2348
/ 631/80/86
/ 692/420
/ Apoptosis
/ Apoptosis Regulatory Proteins - analysis
/ Apoptosis Regulatory Proteins - metabolism
/ Autophagy
/ Beclin-1
/ Biochemistry
/ Biomedical and Life Sciences
/ Cell Biology
/ Cell Cycle Analysis
/ Cell death
/ Cell division
/ Cell Line, Tumor
/ Disease
/ HeLa Cells
/ Humans
/ Kinases
/ Life Sciences
/ Membrane Proteins - analysis
/ Membrane Proteins - metabolism
/ Mitochondria
/ Mitochondria - chemistry
/ Mitochondria - ultrastructure
/ Morphology
/ Mutation
/ Neurodegeneration
/ original-paper
/ Parkinson's disease
/ Protein Kinases - analysis
/ Protein Kinases - genetics
/ Protein Kinases - metabolism
/ Proteins
/ Quality control
/ Sequence Deletion
/ Stem Cells
/ Two-Hybrid System Techniques
2010
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The Parkinson-associated protein PINK1 interacts with Beclin1 and promotes autophagy
by
Michiorri, S
, Giarda, E
, Nerini-Molteni, S
, Russo, M A
, Arena, G
, Torosantucci, L
, Dallapiccola, B
, Lombardi, F
, Marongiu, R
, Casari, G
, Vago, R
, Cassina, L
, Valente, E M
, Romano, F
, Sale, P
, Gelmetti, V
in
631/378/1689/1718
/ 631/80/82/39/2348
/ 631/80/86
/ 692/420
/ Apoptosis
/ Apoptosis Regulatory Proteins - analysis
/ Apoptosis Regulatory Proteins - metabolism
/ Autophagy
/ Beclin-1
/ Biochemistry
/ Biomedical and Life Sciences
/ Cell Biology
/ Cell Cycle Analysis
/ Cell death
/ Cell division
/ Cell Line, Tumor
/ Disease
/ HeLa Cells
/ Humans
/ Kinases
/ Life Sciences
/ Membrane Proteins - analysis
/ Membrane Proteins - metabolism
/ Mitochondria
/ Mitochondria - chemistry
/ Mitochondria - ultrastructure
/ Morphology
/ Mutation
/ Neurodegeneration
/ original-paper
/ Parkinson's disease
/ Protein Kinases - analysis
/ Protein Kinases - genetics
/ Protein Kinases - metabolism
/ Proteins
/ Quality control
/ Sequence Deletion
/ Stem Cells
/ Two-Hybrid System Techniques
2010
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The Parkinson-associated protein PINK1 interacts with Beclin1 and promotes autophagy
Journal Article
The Parkinson-associated protein PINK1 interacts with Beclin1 and promotes autophagy
2010
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Overview
Mutations in the
PINK1
gene cause autosomal recessive Parkinson's disease. The
PINK1
gene encodes a protein kinase that is mitochondrially cleaved to generate two mature isoforms. In addition to its protective role against mitochondrial dysfunction and apoptosis, PINK1 is also known to regulate mitochondrial dynamics acting upstream of the PD-related protein Parkin. Recent data showed that mitochondrial Parkin promotes the autophagic degradation of dysfunctional mitochondria, and that stable PINK1 silencing may have an indirect role in mitophagy activation. Here we report a new interaction between PINK1 and Beclin1, a key pro-autophagic protein already implicated in the pathogenesis of Alzheimer's and Huntington's diseases. Both PINK1 N- and C-terminal are required for the interaction, suggesting that full-length PINK1, and not its cleaved isoforms, interacts with Beclin1. We also demonstrate that PINK1 significantly enhances basal and starvation-induced autophagy, which is reduced by knocking down Beclin1 expression or by inhibiting the Beclin1 partner Vps34. A mutant, PINK1
W437X
, interaction of which with Beclin1 is largely impaired, lacks the ability to enhance autophagy, whereas this is not observed for PINK1
G309D
, a mutant with defective kinase activity but unaltered ability to bind Beclin1. These findings identify a new function of PINK1 and further strengthen the link between autophagy and proteins implicated in the neurodegenerative process.
Publisher
Nature Publishing Group UK,Nature Publishing Group
Subject
/ 692/420
/ Apoptosis Regulatory Proteins - analysis
/ Apoptosis Regulatory Proteins - metabolism
/ Beclin-1
/ Biomedical and Life Sciences
/ Disease
/ Humans
/ Kinases
/ Membrane Proteins - analysis
/ Membrane Proteins - metabolism
/ Mitochondria - ultrastructure
/ Mutation
/ Protein Kinases - metabolism
/ Proteins
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