(Mal) adaptações metabólicas ao treinamento contínuo: concepções não consensuais de terminologia e diagnóstico

Altos desempenhos esportivos demandam treinamentos pesados necessários ao estímulo adaptativo específico a cada esporte. A elevada carga de treino é geralmente acompanhada de discreta fadiga e reduções agudas no desempenho, mas caso acompanhada de períodos apropriados de recuperação, resulta em supercompensação metabólica ao treinamento, refletida como aumento na capacidade aeróbica e/ou força muscular. Visto como contínuo, os processos de intensificação do treinamento e o estresse relacionado à supercompensação, o aumento da sobrecarga ou do estresse poderá, em algum momento, acarretar a quebra da homeostase e a queda temporária da função (supra-alcance - OR ou supra-alcance funcional - FOR). Quando a sobrecarga excessiva de treinamento é combinada com recuperação inadequada há instalação do estado de supratreinamento (OT) ou supra-alcance não funcional (NFOR). O OT excede o OR, cujo pico é também o limiar do OT resultando em desadaptações fisiológicas e queda crônica do desempenho físico. A forma crônica de desadaptação fisiológica ao treinamento físico é chamada de síndrome do supertreinamento (OTS). A própria expressão da síndrome denota a etiologia multifatorial do estado e reconhece que o exercício não é necessariamente seu único fator causal. O diagnóstico de OTS é baseado na recuperação ou não do desempenho. Não há biomarcador objetivo para OTS. A distinção entre OTS e NFOR (supratreinamento extremo) é dependente de desfecho clínico e exclusão diagnóstica de doenças orgânicas, mais comuns na OTS. Também a diferença entre OR e OT é sutil e nenhum de seus marcadores bioquímicos pode ser universalizado. Não há evidências confirmatórias que OR evolui para OT ou que os sintomas de OT são piores dos que os de OR. Apenas pela fadiga aguda e queda de rendimento experimentada em sessões isoladas de treinamento, não é possível diferenciar presentemente os estados de OR e OT. Isto é devido, parcialmente, à variabilidade das respostas individuais ao treinamento e à falta de ambos instrumentos diagnósticos e estudos bem controlados.

Infecção experimental de Mazana gouazoubira (Ficher, 1814) (Cervidae: Odocoileinae) com Haemonchus contortus (Rudolphi, 1803) (Nematoda: Trichostrongyloidea)

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Bioimpedância na gravidez: resistência e reactância de gestantes com pré-eclampsia

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

A função adaptativa da transmissão cultural

O principal objetivo deste artigo é sugerir como podemos explicar a transmissão cultural dentro de um quadro evolucionista geral, aceitável da perspectiva naturalista. Para fazer isso, primeiro reconsiderarei duas das principais teorias que foram propostas com o mesmo objetivo, a saber, a sociobiologia e a memética. Em relação primeira, preservarei a ideia de que a origem dos traços culturais reside em uma adaptação biológica. Relativamente segunda teoria, aceitarei que há um sentido, em que os traços culturais são adaptados, que difere do simples "incremento da fitness biológica". O segundo objetivo, estreitamente relacionado com o primeiro, é explicar porque certos fenômenos culturais não biologicamente adaptativos, as mal-adaptações, mantêm-se e, assim, apresentar um esquema interpretativo adaptacionista, mas não genocêntrico, para a compreensão das dinâmicas culturais. A fim de articular minhas teses em uma proposta original, farei uso das ideias de Boyd e Richerson e introduzirei a distinção entre adaptações de primeira e de segunda ordem.

Western diet changes cardiac acyl-CoA composition in obese rats: a potential role for hepatic lipogenesis.

The "lipotoxic footprint" of cardiac maladaptation in diet-induced obesity is poorly defined. We investigated how manipulation of dietary lipid and carbohydrate influenced potential lipotoxic species in the failing heart. In Wistar rats, contractile dysfunction develops at 48 weeks on a high-fat/high-carbohydrate "Western" diet, but not on low-fat/high-carbohydrate or high-fat diets. Cardiac content of the lipotoxic candidates--diacylglycerol, ceramide, lipid peroxide, and long-chain acyl-CoA species--was measured at different time points by high-performance liquid chromatography and biochemical assays, as was lipogenic capacity in the heart and liver by qRT-PCR and radiometric assays. Changes in membranes fluidity were also monitored using fluorescence polarization. We report that Western feeding induced a 40% decrease in myocardial palmitoleoyl-CoA content and a similar decrease in the unsaturated-to-saturated fatty acid ratio. These changes were associated with impaired cardiac mitochondrial membrane fluidity. At the same time, hepatic lipogenic capacity was increased in animals fed Western diet (+270% fatty acid elongase activity compared with high-fat diet), while fatty acid desaturase activity decreased over time. Our findings suggest that dysregulation of lipogenesis is a significant component of heart failure in diet-induced obesity.

Western diet, but not high fat diet, causes derangements of fatty acid metabolism and contractile dysfunction in the heart of Wistar rats.

Obesity and diabetes are associated with increased fatty acid availability in excess of muscle fatty acid oxidation capacity. This mismatch is implicated in the pathogenesis of cardiac contractile dysfunction and also in the development of skeletal-muscle insulin resistance. We tested the hypothesis that 'Western' and high fat diets differentially cause maladaptation of cardiac- and skeletal-muscle fatty acid oxidation, resulting in cardiac contractile dysfunction. Wistar rats were fed on low fat, 'Western' or high fat (10, 45 or 60% calories from fat respectively) diet for acute (1 day to 1 week), short (4-8 weeks), intermediate (16-24 weeks) or long (32-48 weeks) term. Oleate oxidation in heart muscle ex vivo increased with high fat diet at all time points investigated. In contrast, cardiac oleate oxidation increased with Western diet in the acute, short and intermediate term, but not in the long term. Consistent with fatty acid oxidation maladaptation, cardiac power decreased with long-term Western diet only. In contrast, soleus muscle oleate oxidation (ex vivo) increased only in the acute and short term with either Western or high fat feeding. Fatty acid-responsive genes, including PDHK4 (pyruvate dehydrogenase kinase 4) and CTE1 (cytosolic thioesterase 1), increased in heart and soleus muscle to a greater extent with feeding a high fat diet compared with a Western diet. In conclusion, we implicate inadequate induction of a cassette of fatty acid-responsive genes, and impaired activation of fatty acid oxidation, in the development of cardiac dysfunction with Western diet.

The role of group activity participation in depression among institutionalized elderly

The role of group activity participation in depression among a group of residents (N=65), age 80 and older, in a nursing home was examined using the framework of Roy's Adaptation Theory and Nolen-Hoeksema's Response Style Theory of Depression. Roy views depression as a maladaptation. Nolen-Hoeksema views group activity participation as a therapeutic distraction to break depressed moods and thus allow for positive adaptation. This study utilized data from medical records, group activity attendance, and self-report questionnaires. Demographic distributions were computed and correlational statistics were performed between subjects' participation and their degree of depression, pain experience, functional status, presence of social support, and perception of benefits. Results show a negative correlation between frequency of participation and Geriatric Depression Scale score (GDS). The wide range of measured frequencies among low GDS-scored subjects suggests that less depressed individuals exercise more freedom of choice to participate than those who are more depressed. Significant finding show a positive correlation of group activity participation with functional status in terms of ambulation. Data shows that the experience of pain was not a significant deterrent to participation. The presence of social support from the staff and family did not increase participation. However there is a lesser GDS score among subjects who had recent family/friends visit suggesting a positive role of family in decreasing depression. These results are significant not only for optimizing group therapeutic effects but also for understanding basic human and environmental correlates of depression. Study limitations are pointed out and recommendations are presented.

TRPV4 is necessary for trigeminal irritant pain and functions as a cellular formalin receptor.

Detection of external irritants by head nociceptor neurons has deep evolutionary roots. Irritant-induced aversive behavior is a popular pain model in laboratory animals. It is used widely in the formalin model, where formaldehyde is injected into the rodent paw, eliciting quantifiable nocifensive behavior that has a direct, tissue-injury-evoked phase, and a subsequent tonic phase caused by neural maladaptation. The formalin model has elucidated many antipain compounds and pain-modulating signaling pathways. We have adopted this model to trigeminally innervated territories in mice. In addition, we examined the involvement of TRPV4 channels in formalin-evoked trigeminal pain behavior because TRPV4 is abundantly expressed in trigeminal ganglion (TG) sensory neurons, and because we have recently defined TRPV4's role in response to airborne irritants and in a model for temporomandibular joint pain. We found TRPV4 to be important for trigeminal nocifensive behavior evoked by formalin whisker pad injections. This conclusion is supported by studies with Trpv4(-/-) mice and TRPV4-specific antagonists. Our results imply TRPV4 in MEK-ERK activation in TG sensory neurons. Furthermore, cellular studies in primary TG neurons and in heterologous TRPV4-expressing cells suggest that TRPV4 can be activated directly by formalin to gate Ca(2+). Using TRPA1-blocker and Trpa1(-/-) mice, we found that both TRP channels co-contribute to the formalin trigeminal pain response. These results imply TRPV4 as an important signaling molecule in irritation-evoked trigeminal pain. TRPV4-antagonistic therapies can therefore be envisioned as novel analgesics, possibly for specific targeting of trigeminal pain disorders, such as migraine, headaches, temporomandibular joint, facial, and dental pain, and irritation of trigeminally innervated surface epithelia.

Bases génétiques de la différenciation adaptative en milieu anthropisé chez Macoma balthica, un bivalve marin à fort flux génique

Dans un contexte environnemental anthropisé, fragmenté et soumis à un changement climatique rapide, l’appréhension des processus d'adaptation locale des organismes marins par l'étude de zones de contact entre taxa proches constitue une approche privilégiée. Dans ces zones, des génotypes hybrides persistent malgré un état de maladaptation liée à des incompatibilités génétiques endogènes et/ou des barrières exogènes. L'histoire biogéographique complexe de la telline baltique Macoma balthica fait émerger quatre zones hybrides européennes, dont l'une, localisée autour de la Pointe Finistère (France), est le résultat d’un contact entre deux stocks génétiques ayant divergé en allopatrie. Ces divergences sont susceptibles de rompre la coadaptation entre génomes nucléaire et mitochondrial en raison de l'émergence d'incompatibilités mitonucléaires (MNIs). Ainsi, les sous-unités protéiques des cinq complexes de la chaine OXPHO sont codées à la fois par des gènes nucléaires et mitochondriaux, et une coévolution intergénomique étroite est requise pour maintenir la production énergétique cellulaire. De précédentes données de transcriptomique dévoilent de probables MNIs chez M. balthica au niveau des complexes respiratoires I et V, Afin d’apporter des éléments de compréhension aux mécanismes de maintien des zones hybrides dans un contexte de pression anthropique, le présent travail se propose de tester l'hypothèse de putatives MNIs dans cette zone de contact. Pour cela, (i) six mitogénomes correspondant à cinq lignées haplotypiques divergentes en Europe ont été séquencés et l'architecture génomique a été étudiée conjointement à une cartographie des mutations des 13 gènes mitochondriaux, (ii) le niveau de transcription de 5 gènes nucléaires et 8 gènes mitochondriaux (complexe I à V) des individus hybrides a été comparé à celui des lignées parentales après détermination du statut d'hybridation de chaque individu (six populations françaises). A défaut d'apporter des éléments de réponses concrets quant à l'existence de MNIs chez M. balthica, et ses répercussions évolutives en terme de dépression d'hybridation, ce travail constitue un tremplin vers une étude approfondie de la zone hybride française en développant de nouveaux outils moléculaires, et de solides techniques expérimentales pour la conduite de futurs croisements artificiels.