FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1796740069> ?p ?o ?g. }

• W1796740069 endingPage "415" @default.
• W1796740069 startingPage "355" @default.
• W1796740069 abstract "Alzheimer's disease (AD), Parkinson's disease (PD), and amyotrophic lateral sclerosis (ALS) are the most common human adult-onset neurodegenerative diseases. They are characterized by prominent age-related neurodegeneration in selectively vulnerable neural systems. Some forms of AD, PD, and ALS are inherited, and genes causing these diseases have been identified. Nevertheless, the mechanisms of the neuronal degeneration in these familial diseases, and in the more common idiopathic (sporadic) diseases, are unresolved. Genetic, biochemical, and morphological analyses of human AD, PD, and ALS, as well as their cell and animal models, reveal that mitochondria could have roles in this neurodegeneration. The varied functions and properties of mitochondria might render subsets of selectively vulnerable neurons intrinsically susceptible to cellular aging and stress and the overlying genetic variations. In AD, alterations in enzymes involved in oxidative phosphorylation, oxidative damage, and mitochondrial binding of Aβ and amyloid precursor protein have been reported. In PD, mutations in mitochondrial proteins have been identified and mitochondrial DNA mutations have been found in neurons in the substantia nigra. In ALS, changes occur in mitochondrial respiratory chain enzymes and mitochondrial programmed cell death proteins. Transgenic mouse models of human neurodegenerative disease are beginning to reveal possible principles governing the biology of selective neuronal vulnerability that implicate mitochondria and the mitochondrial permeability transition pore. This chapter reviews several aspects of mitochondrial biology and how mitochondrial pathobiology might contribute to the mechanisms of neurodegeneration in AD, PD, and ALS." @default.
• W1796740069 created "2016-06-24" @default.
• W1796740069 creator A5024878520 @default.
• W1796740069 date "2012-01-01" @default.
• W1796740069 modified "2023-10-05" @default.
• W1796740069 title "Biology of Mitochondria in Neurodegenerative Diseases" @default.
• W1796740069 cites W141294482 @default.
• W1796740069 cites W142080826 @default.
• W1796740069 cites W1497179990 @default.
• W1796740069 cites W1518893426 @default.
• W1796740069 cites W1522890520 @default.
• W1796740069 cites W1524061838 @default.
• W1796740069 cites W1536705765 @default.
• W1796740069 cites W1564677510 @default.
• W1796740069 cites W1573108780 @default.
• W1796740069 cites W1578633669 @default.
• W1796740069 cites W1599584623 @default.
• W1796740069 cites W1618846043 @default.
• W1796740069 cites W1630502818 @default.
• W1796740069 cites W1780295430 @default.
• W1796740069 cites W179329376 @default.
• W1796740069 cites W1873062439 @default.
• W1796740069 cites W1877873625 @default.
• W1796740069 cites W1909302202 @default.
• W1796740069 cites W1937707692 @default.
• W1796740069 cites W1940436875 @default.
• W1796740069 cites W1963947961 @default.
• W1796740069 cites W1965111978 @default.
• W1796740069 cites W1965217295 @default.
• W1796740069 cites W1966134982 @default.
• W1796740069 cites W1966798559 @default.
• W1796740069 cites W1967573239 @default.
• W1796740069 cites W1968257316 @default.
• W1796740069 cites W1968942251 @default.
• W1796740069 cites W1969850018 @default.
• W1796740069 cites W1970094644 @default.
• W1796740069 cites W1971160716 @default.
• W1796740069 cites W1971335269 @default.
• W1796740069 cites W1971639674 @default.
• W1796740069 cites W1972260106 @default.
• W1796740069 cites W1972533526 @default.
• W1796740069 cites W1972812522 @default.
• W1796740069 cites W1972953195 @default.
• W1796740069 cites W1973851166 @default.
• W1796740069 cites W1976475328 @default.
• W1796740069 cites W1976664378 @default.
• W1796740069 cites W1976720365 @default.
• W1796740069 cites W1977069725 @default.
• W1796740069 cites W1977258127 @default.
• W1796740069 cites W1978008790 @default.
• W1796740069 cites W1978119032 @default.
• W1796740069 cites W1978163054 @default.
• W1796740069 cites W1978946171 @default.
• W1796740069 cites W1979179771 @default.
• W1796740069 cites W1979496463 @default.
• W1796740069 cites W1980601652 @default.
• W1796740069 cites W1980959570 @default.
• W1796740069 cites W1981095308 @default.
• W1796740069 cites W1981288814 @default.
• W1796740069 cites W1982029249 @default.
• W1796740069 cites W1982577723 @default.
• W1796740069 cites W1982967923 @default.
• W1796740069 cites W1983030859 @default.
• W1796740069 cites W1984326148 @default.
• W1796740069 cites W1984547206 @default.
• W1796740069 cites W1985773900 @default.
• W1796740069 cites W1986628169 @default.
• W1796740069 cites W1987246914 @default.
• W1796740069 cites W1988849173 @default.
• W1796740069 cites W1988917342 @default.
• W1796740069 cites W1989009610 @default.
• W1796740069 cites W1990284900 @default.
• W1796740069 cites W1990473626 @default.
• W1796740069 cites W1990752558 @default.
• W1796740069 cites W1991548578 @default.
• W1796740069 cites W1993614010 @default.
• W1796740069 cites W1993733276 @default.
• W1796740069 cites W1993772997 @default.
• W1796740069 cites W1994442108 @default.
• W1796740069 cites W1995175521 @default.
• W1796740069 cites W1997858799 @default.
• W1796740069 cites W1998905167 @default.
• W1796740069 cites W2001544013 @default.
• W1796740069 cites W2001614456 @default.
• W1796740069 cites W2005480061 @default.
• W1796740069 cites W2005545438 @default.
• W1796740069 cites W2006925676 @default.
• W1796740069 cites W2007047564 @default.
• W1796740069 cites W2008560382 @default.
• W1796740069 cites W2008748100 @default.
• W1796740069 cites W2009194850 @default.
• W1796740069 cites W2009556855 @default.
• W1796740069 cites W2011284361 @default.
• W1796740069 cites W2011892394 @default.
• W1796740069 cites W2011924331 @default.
• W1796740069 cites W2012014117 @default.
• W1796740069 cites W2012337697 @default.
• W1796740069 cites W2012553386 @default.

• next