RESUMO
Insight on the underlying mechanisms of aging will advance our ability to extend healthspan, treat age-related pathology and improve quality of life. Multiple genetic and pharmacological manipulations extend longevity in different species, yet monotherapy may be relatively inefficient, and we have limited data on the effect of combined interventions. Here we summarize interactions between age-related pathways and discuss strategies to simultaneously retard these in different organisms. In some cases, combined manipulations additively increase their impact on common hallmarks of aging and lifespan, suggesting they quantitatively participate within the same pathway. In other cases, interactions affect different hallmarks, suggesting their joint manipulation may independently maximize their effects on lifespan and healthy aging. While most interaction studies have been conducted with invertebrates and show varying levels of translatability, the conservation of pro-longevity pathways offers an opportunity to identify 'druggable' targets relevant to multiple human age-associated pathologies.
Assuntos
Envelhecimento Saudável , Qualidade de Vida , Humanos , Envelhecimento/genética , Longevidade/genética , Envelhecimento Saudável/genéticaRESUMO
Metabolic flexibility of muscle tissue describes the adaptive capacity to use different energy substrates according to their availability. The disruption of this ability associates with metabolic disease. Here, using a Drosophila model of systemic metabolic dysfunction triggered by yorkie-induced gut tumors, we show that the transcription factor REPTOR is an important regulator of energy metabolism in muscles. We present evidence that REPTOR is activated in muscles of adult flies with gut yorkie-tumors, where it modulates glucose metabolism. Further, in vivo studies indicate that sustained activity of REPTOR is sufficient in wildtype muscles to repress glycolysis and increase tricarboxylic acid (TCA) cycle metabolites. Consistent with the fly studies, higher levels of CREBRF, the mammalian ortholog of REPTOR, reduce glycolysis in mouse myotubes while promoting oxidative metabolism. Altogether, our results define a conserved function for REPTOR and CREBRF as key regulators of muscle energy metabolism.
Assuntos
Proteínas de Drosophila , Drosophila , Metabolismo Energético , Fatores de Transcrição , Proteínas Supressoras de Tumor , Animais , Camundongos , Ciclo do Ácido Cítrico/fisiologia , Glicólise , Músculos/metabolismo , Neoplasias/metabolismo , Proteínas Supressoras de Tumor/genética , Proteínas de Drosophila/genética , Fatores de Transcrição/genéticaRESUMO
Loss of metabolic homeostasis is a hallmark of aging and is characterized by dramatic metabolic reprogramming. To analyze how the fate of labeled methionine is altered during aging, we applied 13C5-Methionine labeling to Drosophila and demonstrated significant changes in the activity of different branches of the methionine metabolism as flies age. We further tested whether targeted degradation of methionine metabolism components would "reset" methionine metabolism flux and extend the fly lifespan. Specifically, we created transgenic flies with inducible expression of Methioninase, a bacterial enzyme capable of degrading methionine and revealed methionine requirements for normal maintenance of lifespan. We also demonstrated that microbiota-derived methionine is an alternative and important source in addition to food-derived methionine. In this genetic model of methionine restriction (MetR), we also demonstrate that either whole-body or tissue-specific Methioninase expression can dramatically extend Drosophila health- and lifespan and exerts physiological effects associated with MetR. Interestingly, while previous dietary MetR extended lifespan in flies only in low amino acid conditions, MetR from Methioninase expression extends lifespan independently of amino acid levels in the food. Finally, because impairment of the methionine metabolism has been previously associated with the development of Alzheimer's disease, we compared methionine metabolism reprogramming between aging flies and a Drosophila model relevant to Alzheimer's disease, and found that overexpression of human Tau caused methionine metabolism flux reprogramming similar to the changes found in aged flies. Altogether, our study highlights Methioninase as a potential agent for health- and lifespan extension.
Assuntos
Drosophila/genética , Longevidade/genética , Metionina/genética , Envelhecimento/genética , Doença de Alzheimer/genética , Aminoácidos/genética , Animais , Animais Geneticamente Modificados/genética , Liases de Carbono-Enxofre/genética , Alimentos , Humanos , Modelos GenéticosRESUMO
Aging is characterized by extensive metabolic reprogramming. To identify metabolic pathways associated with aging, we analyzed age-dependent changes in the metabolomes of long-lived Drosophila melanogaster. Among the metabolites that changed, levels of tyrosine were increased with age in long-lived flies. We demonstrate that the levels of enzymes in the tyrosine degradation pathway increase with age in wild-type flies. Whole-body and neuronal-specific downregulation of enzymes in the tyrosine degradation pathway significantly extends Drosophila lifespan, causes alterations of metabolites associated with increased lifespan, and upregulates the levels of tyrosine-derived neuromediators. Moreover, feeding wild-type flies with tyrosine increased their lifespan. Mechanistically, we show that suppression of ETC complex I drives the upregulation of enzymes in the tyrosine degradation pathway, an effect that can be rescued by tigecycline, an FDA-approved drug that specifically suppresses mitochondrial translation. In addition, tyrosine supplementation partially rescued lifespan of flies with ETC complex I suppression. Altogether, our study highlights the tyrosine degradation pathway as a regulator of longevity.
Assuntos
Envelhecimento/efeitos dos fármacos , Longevidade/fisiologia , Tirosina Transaminase/metabolismo , Tirosina/metabolismo , Tirosina/farmacologia , Animais , Drosophila melanogaster/metabolismo , Complexo de Proteínas da Cadeia de Transporte de Elétrons/efeitos dos fármacos , Longevidade/efeitos dos fármacos , Mitocôndrias/metabolismo , Tigeciclina/farmacologia , Tirosina/análiseRESUMO
Metabolism plays a significant role in the regulation of aging at different levels, and metabolic reprogramming represents a major driving force in aging. Metabolic reprogramming leads to impaired organismal fitness, an age-dependent increase in susceptibility to diseases, decreased ability to mount a stress response, and increased frailty. The complexity of age-dependent metabolic reprogramming comes from the multitude of levels on which metabolic changes can be connected to aging and regulation of lifespan. This is further complicated by the different metabolic requirements of various tissues, cross-organ communication via metabolite secretion, and direct effects of metabolites on epigenetic state and redox regulation; however, not all of these changes are causative to aging. Studies in yeast, flies, worms, and mice have played a crucial role in identifying mechanistic links between observed changes in various metabolic traits and their effects on lifespan. Here, we review how changes in the organismal and organ-specific metabolome are associated with aging and how targeting of any one of over a hundred different targets in specific metabolic pathways can extend lifespan. An important corollary is that restriction or supplementation of different metabolites can change activity of these metabolic pathways in ways that improve healthspan and extend lifespan in different organisms. Due to the high levels of conservation of metabolism in general, translating findings from model systems to human beings will allow for the development of effective strategies for human health- and lifespan extension.
Assuntos
Envelhecimento , Longevidade , Animais , Redes e Vias Metabólicas , Camundongos , Modelos Biológicos , MutaçãoRESUMO
An integrated electrochemical sensing platform is presented, in which stable graphene nanosheets are entrapped within hierarchical gold nano/micro islands (NMI) for the selective detection of dopamine. The fabrication method, which combines lithography, electrodeposition and liquid exfoliation, results in a microscale fluidic reactor capable of handling small volumes (10 µl) of sample. This configuration has advantageous properties, including enhanced sensitivity towards current responses from redox reaction of dopamine to dopamine orthoquinone. The NMIs'spatial orientation inhibits the agglomeration of graphene, while their nanostructured interface enhances adhesion to graphene nanosheets. In turn, this leads to an enlarged surface and to an accumulation of free electrons on the electrode surface. The superior electrocatalytic activity for dopamine is attributed to the high density of π-electrons on graphene nanosheets. In addition, the selectivity of the assay in the presence of other interferents is assumed to be a result of the sp2 π-interactions between the negatively charged graphene layer and the aromatic rings of dopamine. At a working potential of 0.15 V vs Ag/AgCl, the assay has a detection limit of 1.13 nM, a linear range of 1 nM- 100 µM, and apparent recoveries of 106% in spiked synthetic urine. Graphical abstractSchematic presentation of an integrated electrochemical sensing platform, in which stable graphene nanosheets are entrapped within hierarchical gold nano/micro islands (NMI) for selective detection of dopamine. Platinum (Pt) wire and Silver/Silver-Chloride (Ag/AgCl) were used as counter and reference electrode, respectively.
RESUMO
The chalcogenide material MoS2 has been recognized as a promising candidate for photoelectrochemical (PEC) applications due to its enhanced photocatalytic and electrocatalytic activities. However, few reports have been focused on the designated catalytic MoS2 for the nonenzymatic PEC sensing of small molecules. Here, we report on a novel in situ and fab-free method for the direct growth of three-dimensional (3D) porous Peony-like MoS2 nanosheets supported by nanohole-patterned TiO2 and composited with gold deposits. The direct growth resulted in enhanced electrical conductivity between the substrate and 3D-standing MoS2 nanosheets and thus the uniform distribution of gold electrodeposits from the MoS2 lattice. The hybrid 3D MoS2/gold nanocomposite demonstrated enhanced abundance of exposed catalytic edge sites and improved optic and electrical coupling, which ultimately led to excellent photoelectrochemical activities. We performed full characterization of the morphology, crystallinity, lattice configuration, and optical properties of hybrid MoS2 nanosheets via field emission scanning microscope, high-resolution transmission electron microscopy, and energy-dispersive X-ray, Raman, and UV-vis spectroscopies. The 3D COMSOL simulation also confirmed enhanced electric field distribution at the interface of the proposed 3D MoS2/gold nanocomposite electrode in comparison with other morphologies. We acquired the Peony-like 3D MoS2/Au composite for photoelectrochemical sensing of glucose in buffer and diluted plasma solutions with a very low limit of detection of 1.3 nM and superb sensitivity in plasma. Overall, we have successfully synergized both electrical and optical merits from individual components to form a novel composite, which offered an effective scaffold for the development of PEC sensors.
