Fabricio Macedo
Universidade Federal de Sergipe
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Publication
Featured researches published by Fabricio Macedo.
Autonomic Neuroscience: Basic and Clinical | 2012
Larissa Resende Oliveira; Vitor Ulisses de Melo; Fabricio Macedo; André Sales Barreto; Daniel Badaue-Passos; Márcio R. V. Santos; Daniel Penteado Martins Dias; Kathleen A. Sluka; Josimari Melo DeSantana; Valter J. Santana-Filho
Fibromyalgia (FM) is characterized by chronic non-inflammatory widespread pain (CWP) and changes in sympathetic function. In attempt to elucidate the pathophysiological mechanisms of FM we used a well-established CWP animal model. We aimed to evaluate changes in cardiac autonomic balance and baroreflex function in response to CWP induction in rats. CWP was induced by two injections of acidic saline (pH 4.0, n=8) five days apart into the left gastrocnemius muscle. Control animals were injected twice with normal saline (pH 7.2, n=6). One day after the second injection of acidic saline or normal saline, the animals had pulse interval (PI) and systolic arterial pressure (SAP) variability, and spontaneous baroreflex sensitivity (BRS) evaluated. After induction of CWP, there was an increase of power in the low frequency (LF) band of PI spectrum (12.75 ± 1.04 nu), a decrease in the high frequency (HF) band (87.25 ± 1.04 nu) and an increase of LF/HF ratio (0.16 ± 0.01), when compared to control animals (7.83 ± 1.13 nu LF; 92.16 ± 1.13 nu HF; 0.08 ± 0.01 LF/HF). In addition, there was an increase of power in the LF band of SAP spectrum (7.93 ± 1.39 mmHg(2)) when compared to control animals (2.97 ± 0.61 mmHg(2)). BRS was lower in acidic saline injected rats (0.59 ± 0.06 ms/mmHg) when compared to control animals (0.71 ± 0.03 ms/mmHg). Our results showed that induction of CWP in rats shifts cardiac sympathovagal balance towards sympathetic predominance and decreases BRS. These data corroborate findings in humans with FM.
Frontiers in Physiology | 2016
Fabricio Macedo; Thássio Ricardo Ribeiro Mesquita; V.U. Melo; Marcelo Mendonça Mota; Tharciano Luiz Teixeira Braga da Silva; Michael Nadson Santos Santana; Larissa Resende Oliveira; Robervan Vidal Santos; Rodrigo Miguel dos Santos; Sandra Lauton-Santos; Márcio R. V. Santos; André Sales Barreto; Valter J. Santana-Filho
Resistance training is one of the most common kind of exercise used nowadays. Long-term high-intensity resistance training are associated with deleterious effects on vascular adjustments. On the other hand, is unclear whether low-intensity resistance training (LI-RT) is able to induce systemic changes in vascular tone. Thus, we aimed to evaluate the effects of chronic LI-RT on endothelial nitric oxide (NO) bioavailability of mesenteric artery and cardiovascular autonomic modulation in healthy rats. Wistar animals were divided into two groups: exercised (Ex) and sedentary (SED) rats submitted to the resistance (40% of 1RM) or fictitious training for 8 weeks, respectively. After LI-RT, hemodynamic measurements and cardiovascular autonomic modulation by spectral analysis were evaluated. Vascular reactivity, NO production and protein expression of endothelial and neuronal nitric oxide synthase isoforms (eNOS and nNOS, respectively) were evaluated in mesenteric artery. In addition, cardiac superoxide anion production and ventricle morphological changes were also assessed. In vivo measurements revealed a reduction in mean arterial pressure and heart rate after 8 weeks of LI-RT. In vitro studies showed an increased acetylcholine (ACh)-induced vasorelaxation and greater NOS dependence in Ex than SED rats. Hence, decreased phenylephrine-induced vasoconstriction was found in Ex rats. Accordingly, LI-RT increased the NO bioavailability under basal and ACh stimulation conditions, associated with upregulation of eNOS and nNOS protein expression in mesenteric artery. Regarding autonomic control, LI-RT increased spontaneous baroreflex sensitivity, which was associated to reduction in both, cardiac and vascular sympathetic modulation. No changes in cardiac superoxide anion or left ventricle morphometric parameters after LI-RT were observed. In summary, these results suggest that RT promotes beneficial vascular adjustments favoring augmented endothelial NO bioavailability and reduction of sympathetic vascular modulation, without evidence of cardiac overload.
Frontiers in Pharmacology | 2017
Thássio Ricardo Ribeiro Mesquita; Itamar Couto Guedes de Jesus; Jucilene F. dos Santos; Grace Kelly Melo de Almeida; Carla Maria Lins de Vasconcelos; Silvia Guatimosim; Fabricio Macedo; Robervan Santos; José Evaldo Rodrigues de Menezes-Filho; Rodrigo Miguel-dos-Santos; Paulo Tojal Dantas Matos; Sergio Scalzo; Valter J. Santana-Filho; Ricardo Luiz Cavalcanti De Albuquerque-Júnior; Rose Nely Pereira-Filho; Sandra Lauton-Santos
Ginkgo biloba is the most popular phytotherapic agent used worldwide for treatment of several human disorders. However, the mechanisms involved in the protective actions of Ginkgo biloba on cardiovascular diseases remain poorly elucidated. Taking into account recent studies showing beneficial actions of cholinergic signaling in the heart and the cholinergic hypothesis of Ginkgo biloba-mediated neuroprotection, we aimed to investigate whether Ginkgo biloba extract (GBE) promotes cardioprotection via activation of cholinergic signaling in a model of isoproterenol-induced cardiac hypertrophy. Here, we show that GBE treatment (100 mg/kg/day for 8 days, v.o.) reestablished the autonomic imbalance and baroreflex dysfunction caused by chronic β-adrenergic receptor stimulation (β-AR, 4.5 mg/kg/day for 8 days, i.p.). Moreover, GBE prevented the upregulation of muscarinic receptors (M2) and downregulation of β1-AR in isoproterenol treated-hearts. Additionally, we demonstrated that GBE prevents the impaired endothelial nitric oxide synthase activity in the heart. GBE also prevented the pathological cardiac remodeling, electrocardiographic changes and impaired left ventricular contractility that are typical of cardiac hypertrophy. To further investigate the mechanisms involved in GBE cardioprotection in vivo, we performed in vitro studies. By using neonatal cardiomyocyte culture we demonstrated that the antihypertrophic action of GBE was fully abolished by muscarinic receptor antagonist or NOS inhibition. Altogether, our data support the notion that antihypertrophic effect of GBE occurs via activation of M2/NO pathway uncovering a new mechanism involved in the cardioprotective action of Ginkgo biloba.
The FASEB Journal | 2015
Fabricio Macedo; Thássio Ricardo Ribeiro Mesquita; Vitor Ulisses de Melo; Rodrigo Miguel dos Santos; Michael Nadson Santos Santana; Robervan Santos; Larissa Resende Oliveira; Marcelo Mendonça Mota; Tharciano Luiz Teixeira Braga da Silva; André Sales Barreto; Márcio R. V. Santos; Sandra Lauton-Santos; Valter J. Santana-Filho
The FASEB Journal | 2015
Elizabete Silva-Filha; Tamires Costa; Bruna Farias; Polyana Santos; Michael Nadson Santos Santana; Fabricio Macedo; Robervan Santos; Valter J. Santana-Filho
Autonomic Neuroscience: Basic and Clinical | 2015
Valter J. Santana-Filho; V.U. Melo; Rayssa Rizerio de Moura Saldanha; Fabricio Macedo; Michael Nadson Santos Santana; Larissa Resende Oliveira; Robervan Vidal Santos; André Sales Barreto; Márcio R. V. Santos; J. C. Cruz; Santos Cr; Lisete C. Michelini
The FASEB Journal | 2014
Larissa Resende Oliveira; Fabricio Macedo; Vitor Ulisses de Melo; Marcelo Mendonça Mota; Tharciano Luiz Teixeira Braga da Silva; Milene Tavares Fontes; Michael Nadson Santos Santana; Robervan Santos; André Sales Barreto; Márcio Roberto dos Santos; Valter J. Santana-Filho
The FASEB Journal | 2013
Mario Matiotti Neto; Robervan Vidal Santos; V.U. Melo; Fabricio Macedo; Jose Luiz de Brito Alves; Márcio R. V. Santos; Larissa Resende Oliveira; Michael Nadson Santos Santana; Luciana C. Brito; João Silva; Elizabeth Nasciment; Pauliana Ribeiro dos Santos
The FASEB Journal | 2013
Robervan Santos; Vitor Melo; Fabricio Macedo; Jose Luiz de Brito Alves; Márcio R. V. Santos; Larissa Resende Oliveira; Michael Nadson Santos Santana; Mario Matiotti; Luciana C. Brito; Elizabeth Nascimento; João Silva; Valter J. Santana-Filho
The FASEB Journal | 2012
Fabricio Macedo; Vitor Ulisses de Melo; Michael Nadson Santos Santana; Katielle Messenger Oliveira; Larissa Resende Oliveira; Márcio R. V. Santos; Daniel Badaue-Passos; André Sales Barreto; Valter J. Santana-Filho