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Neurons share more similarities with insulin-producing pancreatic
islet cells than with any other cell type. The root of this
similarity may lie in the islet's evolution from an ancestral
insulin-producing neuron. The islet-neuron connection becomes less
surprising as we learn more about insulin's involvement in
functions far from its traditional role in mediating glucose uptake
in muscle. The importance of insulin in the regulation of corporal
aging has been established by the dramatic increases in longevity
experienced by animals in which the adipose insulin receptor has
been genetically eliminated, or in which the insulin-related daf
genes have been mutated. New research suggests that, analogous to
its influence on corporal aging, insulin also makes important
contributions to brain aging and the expression of late-life
neurodegenerative disease. Insulin plays a key role in cognition
and other aspects of normal brain function. Insulin resistance
induces chronic peripheral insulin elevations and is associated
with reduced insulin activity both in periphery and brain. The
insulin resistance syndrome underlies conditions such as Type 2
diabetes mellitus and hypertension, which are associated with
age-related cognitive impairment and Alzheimer's disease. This book
discusses the mechanisms through which insulin dysregulation
contributes to the development of cognitive impairment and
late-life neurodegenerative disease. Given the recent pandemic of
conditions associated with insulin resistance, it is imperative
that we achieve a comprehensive knowledge of the mechanisms through
which insulin resistance affects brain function in order to develop
therapeutic strategies to address these effects.
The central nervous system controls vital functions by ef?ciently
coordinating peripheral and central cascades of signals and
networks in an orchestrated manner. Historically, the brain was
considered to be insulin independent. These earlier views have been
challenged by ?ndings demonstrating that insulin exerts multiple
actions in the brain, regulating vital biological processes such as
life span, neuronal survival, cognition, reproduction, feeding
behavior, energy balance, and glucose and fat metabolism, and that
inef?cient central action of insulin contributes to the development
of severe pathologies (Banks et al. 2000; Gerozissis 2003, 2004,
2008; Lustman and Clouse 2005; Okamoto et al. 2001; Park 2002;
Perrin et al. 2004; Pocai et al. 2005; Reger et al. 2008; Schwartz
and Porte, 2005; Schubert et al. 2004; van der Heide et al. 2005;
Woods et al. 1979; Wrighten et al. 2008). Insulin and speci?c
insulin receptors are widely distributed in the networks of the
central nervous system related mainly to feeding or cognition
(Baskin et al. 1983; Bruning et al. 2000; Gerozissis 2003, 2008;
Havrankova et al. 1978a, b; Schechter et al. 1996; Schulingkamp et
al. 2000; Schwartz et al. 1992; Zhao et al. 2004). Insulin
receptors located in the synapses of neurons and in astrocytes are
present in high concentrations in the cerebral cortex, olfactory
bulb, hippocampus, amygdala, cerebellum and hypothalamus (Abbott et
al., 1999; Havrankova et al.
Ausbau und Verstetigung einer inklusiven Bildungsinfrastruktur fur
das Lernen Erwachsener sind dezidierte Aufgaben offentlicher
Weiterbildung. Grundversorgung, Zuganglichkeit und
Bildungsgerechtigkeit signalisieren die politisch-gesellschaftliche
Dimension der Aufgabenstellung, ein effizientes Management die
okonomische Dimension. Beide Perspektiven stehen im Zentrum dieses
Bandes, der Klaus Meisel zum 60. Geburtstag gewidmet ist.
Engagierte Beweglichkeit kann in institutioneller Perspektive als
gleichzeitige Fokussierung auf Infrastruktur- und
Angebotsgestaltung fur das Lernen Erwachsener und auf
wirtschaftliche Ressourcenoptimierung und Sparsamkeit gedeutet
werden. In professioneller Perspektive verweist sie auf das
habitualisierte Handeln der verantwortlichen Akteure, die nicht nur
die Gestaltung des Lernens, sondern auch die Gestaltung in und an
der Organisation in Bewegung bringen. "
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