Your search keyword '"Santos MD"' showing total 9 results

1. Lactobacillus paracasei modulates the immune system of Galleria mellonella and protects against Candida albicans infection.

Author

Rossoni RD, Fuchs BB, de Barros PP, Velloso MD, Jorge AO, Junqueira JC, and Mylonakis E

Subjects

Animals, Colony Count, Microbial, Gene Expression Regulation, Hemocytes, Hemolymph, Host-Pathogen Interactions genetics, Host-Pathogen Interactions immunology, Humans, Larva microbiology, Moths genetics, Probiotics, Candida albicans immunology, Disease Resistance immunology, Immunomodulation, Lacticaseibacillus paracasei physiology, Moths immunology, Moths microbiology

Abstract

Probiotics have been described as a potential strategy to control opportunistic infections due to their ability to stimulate the immune system. Using the non-vertebrate model host Galleria mellonella, we evaluated whether clinical isolates of Lactobacillus spp. are able to provide protection against Candida albicans infection. Among different strains of Lactobacillus paracasei, Lactobacillus rhamnosus and Lactobacillus fermentum, we verified that L. paracasei 28.4 strain had the greatest ability to prolong the survival of larvae infected with a lethal dose of C. albicans. We found that the injection of 107 cells/larvae of L. paracasei into G. mellonella larvae infected by C. albicans increased the survival of these insects compared to the control group (P = 0.0001). After that, we investigated the immune mechanisms involved in the protection against C. albicans infection, evaluating the number of hemocytes and the gene expression of antifungal peptides. We found that L. paracasei increased the hemocyte quantity (2.38 x 106 cells/mL) in relation to the control group (1.29 x 106 cells/mL), indicating that this strain is capable of raising the number of circulating hemocytes into the G. mellonella hemolymph. Further, we found that L. paracasei 28.4 upregulated genes that encode the antifungal peptides galiomicin and gallerymicin. In relation to the control group, L. paracasei 28.4 increased gene expression of galiomicin by 6.67-fold and 17.29-fold for gallerymicin. Finally, we verified that the prophylactic provision of probiotic led to a significant reduction of the number of fungal cells in G. mellonella hemolymph. In conclusion, L. paracasei 28.4 can modulate the immune system of G. mellonella and protect against candidiasis.

Published

2017

2. Comparative Cytogenetics between Two Important Songbird, Models: The Zebra Finch and the Canary.

Author

Dos Santos MD, Kretschmer R, Frankl-Vilches C, Bakker A, Gahr M, O Brien PC, Ferguson-Smith MA, and de Oliveira EH

Subjects

Animals, Chickens genetics, Chromosome Inversion genetics, Chromosome Painting, Genomics, In Situ Hybridization, Fluorescence, Karyotype, Karyotyping, Canaries genetics, Cytogenetics, Evolution, Molecular, Finches genetics

Abstract

Songbird species (order Passeriformes, suborder Oscines) are important models in various experimental fields spanning behavioural genomics to neurobiology. Although the genomes of some songbird species were sequenced recently, the chromosomal organization of these species is mostly unknown. Here we focused on the two most studied songbird species in neuroscience, the zebra finch (Taeniopygia guttata) and the canary (Serinus canaria). In order to clarify these issues and also to integrate chromosome data with their assembled genomes, we used classical and molecular cytogenetics in both zebra finch and canary to define their chromosomal homology, localization of heterochromatic blocks and distribution of rDNA clusters. We confirmed the same diploid number (2n = 80) in both species, as previously reported. FISH experiments confirmed the occurrence of multiple paracentric and pericentric inversions previously found in other species of Passeriformes, providing a cytogenetic signature for this order, and corroborating data from in silico analyses. Additionally, compared to other Passeriformes, we detected differences in the zebra finch karyotype concerning the morphology of some chromosomes, in the distribution of 5S rDNA clusters, and an inversion in chromosome 1., Competing Interests: The authors have declared that no competing interests exist.

Published

2017

3. Selenium and Zinc Status in Chronic Myofascial Pain: Serum and Erythrocyte Concentrations and Food Intake.

Author

Barros-Neto JA, Souza-Machado A, Kraychete DC, Jesus RP, Cortes ML, Lima MD, Freitas MC, Santos TM, Viana GF, and Menezes-Filho JA

Subjects

Adult, Alcohol Drinking, Body Mass Index, Case-Control Studies, Chronic Disease, Diet, Exercise, Female, Hemoglobins analysis, Humans, Life Style, Male, Middle Aged, Nutritional Status, Selenium analysis, Smoking, Zinc analysis, Eating physiology, Erythrocytes chemistry, Pain pathology, Selenium blood, Zinc blood

Abstract

Introduction: Nutritional disorders have been reported to be important causal factors that can intensify or cause a painful response in individuals with chronic musculoskeletal pain., Aim: To assess the habitual intake of and the serum and erythrocyte levels of selenium and zinc in patients with chronic myofascial pain., Materials and Methods: A case-control study of 31 patients with chronic myofascial pain (group I) and 31 subjects without pain (group II). Dietary record in five days for assessing food intake were used. The serum and erythrocyte concentrations of selenium and zinc were analyzed using an atomic absorption spectrophotometry. Pain intensity was assessed using a visual analog scale., Results: The group of patients with chronic myofascial pain, compared with the control group, showed a lower erythrocyte concentration of selenium (79.46 ± 19.79 μg/L vs. 90.80 ± 23.12 μg/L; p = 0.041) and zinc (30.56 ± 7.74 μgZn/gHb vs. 38.48 ± 14.86 μgZn/gHb, respectively; p = 0.004). In this study, a compromised food intake of zinc was observed in the majority of the subjects in both groups. The selenium intake was considered to be safe in 80% of the subjects in both groups; however, the likelihood of inadequate intake of this mineral was twice as high in group I (49.5% vs. 24.4%, respectively). In the logistic regression analysis, the erythrocyte concentration of zinc was associated with the presence of pain. In each additional 1 mg of Zn2+ per gram of hemoglobin, a reduction of 12.5% was observed in the risk of the individual having chronic myofascial pain (B = -0.133; adjusted OR = 0.875, 95% CI = 0.803 to 0.954, Wald = 9.187, standard error = 0.044, p = 0.002). Physical inactivity and obesity were noted more commonly in group I compared with the control group., Conclusion: In this study, patients with chronic myofascial pain showed lower intracellular stores of zinc and selenium and inadequate food intake of these nutrients., Competing Interests: The authors have declared that no competing interests exist.

Published

2016

4. Correction: Distinct Yellowfin Tuna (Thunnus albacares) Stocks Detected in Western and Central Pacific Ocean (WCPO) Using DNA Microsatellites.

Author

Aguila RD, Perez SK, Catacutan BJ, Lopez GV, Barut NC, and Santos MD

Published

2015

5. Distinct Yellowfin Tuna (Thunnus albacares) Stocks Detected in Western and Central Pacific Ocean (WCPO) Using DNA Microsatellites.

Author

Aguila RD, Perez SK, Catacutan BJ, Lopez GV, Barut NC, and Santos MD

Subjects

Animals, Genetic Loci, Genetic Markers genetics, Muscle, Skeletal metabolism, Pacific Ocean, Papua New Guinea, Philippines, Polymerase Chain Reaction, Principal Component Analysis, Species Specificity, Microsatellite Repeats genetics, Tuna genetics

Abstract

The yellowfin tuna, Thunnus albacares (Bonnaterre, 1788), covers majority of the Philippines' tuna catch, one of the major fisheries commodities in the country. Due to its high economic importance sustainable management of these tunas has become an imperative measure to prevent stock depletion. Currently, the Philippine yellowfin tuna is believed to be part of a single stock of the greater WCPO though some reports suggest otherwise. This study therefore aims to establish the genetic stock structure of the said species in the Philippines as compared to Bismarck Sea, Papua New Guinea using nine (9) DNA microsatellite markers. DNA microsatellite data revealed significant genetic differentiation between the Philippine and Bismarck Sea, Papua New Guinea yellowfin tuna samples. (FST = 0.034, P = 0.016), which is further supported by multilocus distance matrix testing (PCoA) and model-based clustering (STRUCTURE 2.2).With these findings, this study posits that the yellowfin tuna population in the Philippines is a separate stock from the Bismarck Sea population. These findings add evidence to the alternative hypothesis of having at least 2 subpopulations of yellowfin tuna in the WCPO and calls for additional scientific studies using other parameters to investigate this. Accurate population information is necessary in formulating a more appropriate management strategy for the sustainability of the yellowfin tuna not only in the Philippines but also in the WCPO.

Published

2015

6. Dynamics of CRISPR loci in microevolutionary process of Yersinia pestis strains.

Author

Barros MP, França CT, Lins RH, Santos MD, Silva EJ, Oliveira MB, Silveira-Filho VM, Rezende AM, Balbino VQ, and Leal-Balbino TC

Subjects

5' Untranslated Regions genetics, Base Sequence, Brazil, DNA, Bacterial analysis, Evolution, Molecular, Genes, Bacterial, Genetic Variation, Genome, Bacterial, Genotype, Molecular Sequence Data, Phylogeny, Plague microbiology, Sequence Analysis, DNA, Yersinia pestis classification, Yersinia pseudotuberculosis genetics, Clustered Regularly Interspaced Short Palindromic Repeats genetics, DNA, Bacterial genetics, DNA, Intergenic genetics, Yersinia pestis genetics

Abstract

The potential use of CRISPR loci genotyping to elucidate population dynamics and microevolution of 146 Yersinia pestis strains from different biovars and locations was investigated in this work. The majority of strains from the Orientalis biovar presented specific spacer arrays, allowing for the establishment of a CRISPR signature for their respective isolates. Twenty-one new spacers were found in the Y. pestis strains from plague foci in Brazil. Ninety-three (64%) strains were grouped in the G1 genotype, whereas the others were distributed in 35 genotypes. This study allowed observing a microevolutionary process in a group of Y. pestis isolated from Brazil. We also identified specific genotypes of Y. pestis that were important for the establishment of the bacteria in plague foci in Brazil. The data have provided supporting evidence for the diversity and dynamics of CRISPR loci present in the genome of Y. pestis strains from plague foci in Brazil.

Published

2014

7. Hidden diversity in sardines: genetic and morphological evidence for cryptic species in the goldstripe sardinella, Sardinella gibbosa (Bleeker, 1849).

Author

Thomas RC Jr, Willette DA, Carpenter KE, and Santos MD

Subjects

Animals, Cell Nucleus genetics, Genetic Markers genetics, Genotyping Techniques, Likelihood Functions, Mitochondria genetics, Fishes anatomy & histology, Fishes genetics, Genetic Variation, Phylogeny

Abstract

Cryptic species continue to be uncovered in many fish taxa, posing challenges for fisheries conservation and management. In Sardinella gibbosa, previous investigations revealed subtle intra-species variations, resulting in numerous synonyms and a controversial taxonomy for this sardine. Here, we tested for cryptic diversity within S. gibbosa using genetic data from two mitochondrial and one nuclear gene regions of 248 individuals of S. gibbosa, collected from eight locations across the Philippine archipelago. Deep genetic divergence and subsequent clustering was consistent across both mitochondrial and nuclear markers. Clade distribution is geographically limited: Clade 1 is widely distributed in the central Philippines, while Clade 2 is limited to the northernmost sampling site. In addition, morphometric analyses revealed a unique head shape that characterized each genetic clade. Hence, both genetic and morphological evidence strongly suggests a hidden diversity within this common and commercially-important sardine.

Published

2014

8. Discrimination of juvenile yellowfin (Thunnus albacares) and bigeye (T. obesus) Tunas using mitochondrial DNA control region and liver morphology.

Author

Pedrosa-Gerasmio IR, Babaran RP, and Santos MD

Subjects

Animals, Genetic Markers, Molecular Typing, Phenotype, Phylogeny, Principal Component Analysis, Sequence Analysis, DNA, Tuna anatomy & histology, Tuna genetics, DNA, Mitochondrial genetics, Liver anatomy & histology, Regulatory Sequences, Nucleic Acid, Tuna classification

Abstract

Yellowfin tuna, Thunnus albacares (Bonnaterre, 1788) and bigeye tuna, Thunnus obesus (Lowe, 1839) are two of the most economically important tuna species in the world. However, identification of their juveniles, especially at sizes less than 40 cm, is very difficult, often leading to misidentification and miscalculation of their catch estimates. Here, we applied the mitochondrial DNA control region D-loop, a recently validated genetic marker used for identifying tuna species (Genus Thunnus), to discriminate juvenile tunas caught by purse seine and ringnet sets around fish aggregating devices (FADs) off the Southern Iloilo Peninsula in Central Philippines. We checked individual identifications using the Neighbor-Joining Method and compared results with morphometric analyses and the liver phenotype. We tested 48 specimens ranging from 13 to 31 cm fork length. Morpho-meristic analyses suggested that 12 specimens (25%) were bigeye tuna and 36 specimens (75%) were yellowfin tuna. In contrast, the genetic and liver analyses both showed that 5 specimens (10%) were bigeye tuna and 43 (90%) yellowfin tuna. This suggests that misidentification can occur even with highly stringent morpho-meristic characters and that the mtDNA control region and liver phenotype are excellent markers to discriminate juveniles of yellowfin and bigeye tunas.

Published

2012

9. Dendritic hold and read: a gated mechanism for short term information storage and retrieval.

Author

Santos MD, Mohammadi MH, Yang S, Liang CW, Kao JP, Alger BE, Thompson SM, and Tang CM

Subjects

Animals, Rats, Rats, Sprague-Dawley, Receptors, N-Methyl-D-Aspartate metabolism, Synapses metabolism, Synaptic Transmission physiology, Dendrites physiology, Memory, Short-Term physiology, Models, Neurological, Neuronal Plasticity physiology, Neurons physiology

Abstract

Two contrasting theories have been proposed to explain the mechanistic basis of short term memory. One theory posits that short term memory is represented by persistent neural activity supported by reverberating feedback networks. An alternate, more recent theory posits that short term memory can be supported by feedforward networks. While feedback driven memory can be implemented by well described mechanisms of synaptic plasticity, little is known of possible molecular and cellular mechanisms that can implement feedforward driven memory. Here we report such a mechanism in which the memory trace exists in the form of glutamate-bound but Mg(2+)-blocked NMDA receptors on the thin terminal dendrites of CA1 pyramidal neurons. Because glutamate dissociates from subsets of NMDA receptors very slowly, excitatory synaptic transmission can leave a silent residual trace that outlasts the electrical activity by hundreds of milliseconds. Read-out of the memory trace is possible if a critical level of these bound-but-blocked receptors accumulates on a dendritic branch that will allow these quasi-stable receptors to sustain a regenerative depolarization when triggered by an independent gating signal. This process is referred to here as dendritic hold and read (DHR). Because the read-out of the input is not dependent on repetition of the input and information flows in a single-pass manner, DHR can potentially support a feedforward memory architecture.

Published

2012