Proteins of nucleotide and base excision repair pathways interact in mitochondria to protect from loss of subcutaneous fat, a hallmark of aging

Kamenisch, York; Fousteri, Maria; Knoch, Jennifer; Thaler, Anna Katharina Von; Fehrenbacher, Birgit; Kato, Hiromichi; Becker, Thomas; Dollé, Martijn E.T.; Kuiper, Raoul V.; Majora, Marc; Schaller, Martin; Horst, Gijsbertus T. J. van der; Steeg, Harry van; Röcken, Martin; Rapaport, Doron; Krutmann, Jean; Mullenders, Leon H.F.; Berneburg, Mark

doi:10.1084/jem.20091834

Cited by 156 publications

(146 citation statements)

References 45 publications

(104 reference statements)

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“…Oxidative stress has been observed in several neurodegenerative diseases (Trushina and McMurray, 2007), providing a link between our findings of increased ROS production and decreased autophagy to the neuropathology seen in CS. These findings could also explain the accumulation of lesions found in mitochondria from CSB deficient cells (Muftuoglu et al, 2009;Osenbroch et al, 2009;Aamann et al, 2010;Kamenisch et al, 2010). The in creased oxygen and glucose consumption we observe indicates a state of cellular energy deprivation.…”

Section: Mrisupporting

confidence: 52%

“…CSB localizes to the mitochondria and interacts with the nucle oid, especially under conditions of oxidative stress (Aamann et al, 2010;Kamenisch et al, 2010). We hypothesize that CSB plays a role as a sensor of mtDNA damage, either by directly binding to mtDNA or as an indirect signaling protein.…”

Section: Discussionmentioning

confidence: 94%

“…Endogenous oxidizing radicals originate pre dominantly from the mitochondria, where the mitochondrial BER machinery acts as the pri mary protector. Recent findings indicate that CSB is present in the mitochondria, suggesting a role for CSB in mitochondrial DNA (mtDNA) repair (Aamann et al, 2010;Kamenisch et al, 2010). We now report that CSB participates in mitochondrial maintenance by inducing…”

mentioning

confidence: 80%

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Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy

Scheibye‐Knudsen¹,

Ramamoorthy²,

Sýkora³

et al. 2012

J Cell Biol

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Section: Mrisupporting

confidence: 52%

Section: Discussionmentioning

confidence: 94%

mentioning

confidence: 80%

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Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy

Scheibye‐Knudsen¹,

Ramamoorthy²,

Sýkora³

et al. 2012

J Cell Biol

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“…Suggestions have been made that CS caused by faulty responses to endogenously generated oxidative damage through additional deficiencies in base excision repair (18), mitochondrial activity (22), and coordination of a transcriptional response (4,23). However, although CSA and CSB patients have indistinguishable clinical disease, only CSB and not CSA or UV s cells are sensitive to oxidative damage (14,17,24).…”

mentioning

confidence: 99%

Dysmyelination not demyelination causes neurological symptoms in preweaned mice in a murine model of Cockayne syndrome

Revet¹,

Feeney²,

Tang³

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Cockayne syndrome (CS) is a rare autosomal recessive neurodegenerative disease that is associated with mutations in either of two transcription-coupled DNA repair genes, CSA or CSB. oligodendrocytes were unable to generate sufficient MBP or to maintain the proper myelination during early development. Csb is a multifunctional protein regulating both repair and the transcriptional response to reactive oxygen through its interaction with histone acetylase p300 and the hypoxia-inducible factor (HIF)1 pathway. On the basis of our results, combined with that of others, we suggest that in Csb the transcriptional response predominates during early development, whereas a neurodegenerative response associated with repair deficits predominates in later life.transcription-coupled repair | behavior | rotenone | γH2Ax

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“…Além disso, recentemente foi descrita a presença de CSA e CSB na mitocôndria (Aamann et al, 2010;Kamenisch et al, 2010), onde essas proteínas parecem ser importantes no reparo do mtDNA, assim como na manutenção do estado redox das células (Pascucci et al, 2012). Dessa forma, ainda não há certeza sobre qual o mecanismo mais importante na patologia (principalmente neurológica) de CS, se são as deficiências no reparo ou na transcrição (Brooks, 2013), ou um mecanismo conjunto (Jaarsma et al, 2011); além disso, no caso da deficiência de reparo, também existe controvérsia sobre qual seria o tipo de dano responsável pela patologia neurológica (Cleaver et al, 2013).…”

Section: Cs é Causada Por Mutações Nos Genes Csa/ercc8 (35% Dos Casosunclassified

Papel das proteínas XPD e DNA polimerase eta nas respostas de células humanas a danos no genoma

Lerner¹

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Proteins of nucleotide and base excision repair pathways interact in mitochondria to protect from loss of subcutaneous fat, a hallmark of aging

Cited by 156 publications

References 45 publications

Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy

Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy

Dysmyelination not demyelination causes neurological symptoms in preweaned mice in a murine model of Cockayne syndrome

Papel das proteínas XPD e DNA polimerase eta nas respostas de células humanas a danos no genoma

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