Search

Your search keyword '"Candela M"' showing total 1,005 results
Start Over Author "Candela M"
1,005 results on '"Candela M"'

101. Early gut microbiota signature of aGvHD in children given allogeneic hematopoietic cell transplantation for hematological disorders

Author

Biagi, E., Zama, D., Rampelli, S., Turroni, S., Brigidi, P., Consolandi, C., Severgnini, M., Picotti, E., Gasperini, P., Merli, P., Decembrino, N., Zecca, M., Cesaro, S., Faraci, M., Prete, A., Locatelli, Franco, Pession, A., Candela, M., Masetti, R., Locatelli F. (ORCID:0000-0002-7976-3654), Biagi, E., Zama, D., Rampelli, S., Turroni, S., Brigidi, P., Consolandi, C., Severgnini, M., Picotti, E., Gasperini, P., Merli, P., Decembrino, N., Zecca, M., Cesaro, S., Faraci, M., Prete, A., Locatelli, Franco, Pession, A., Candela, M., Masetti, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: The onset of acute Graft-versus-Host Disease (aGvHD) has been correlated with the gut microbiota (GM) composition, but experimental observations are still few, mainly involving cohorts of adult patients. In the current scenario where fecal microbiota transplantation has been used as a pioneer therapeutic approach to treat steroid-refractory aGvHD, there is an urgent need to expand existing observational studies of the GM dynamics in Hematopoietic Stem Cell Transplantation (HSCT). Aim of the present study is to explore the GM trajectory in 36 pediatric HSCT recipients in relation to aGvHD onset. Methods: Thirty-six pediatric patients, from four transplantation centers, undergoing HSCT were enrolled in the study. Stools were collected at three time points: before HSCT, at time of engraftment and > 30 days following HSCT. Changes in the GM phylogenetic structure were studied by 16S rRNA gene Illumina sequencing and phylogenetic assignation. Results: Children developing gut aGvHD had a dysbiotic GM layout before HSCT occurred. This putative aGvHD-predisposing ecosystem state was characterized by (i) reduced diversity, (ii) lower Blautia content, (iii) increase in Fusobacterium abundance. At time of engraftment, the GM structure underwent a deep rearrangement in all patients but, regardless of the occurrence of aGvHD and its treatment, it reacquired a eubiotic configuration from day 30. Conclusions: We found a specific GM signature before HSCT predictive of subsequent gut aGvHD occurrence. Our data may open the way to a GM-based stratification of the risk of developing aGvHD in children undergoing HSCT, potentially useful also to identify patients benefiting from prophylactic fecal transplantation.

Published
2019

117. Microbiomes of Thalassia testudinum throughout the Atlantic Ocean, Caribbean Sea, and Gulf of Mexico are influenced by site and region while maintaining a core microbiome

Author

Kelly Ugarelli, Justin E. Campbell, O. Kennedy Rhoades, Calvin J. Munson, Andrew H. Altieri, James G. Douglass, Kenneth L. Heck, Valerie J. Paul, Savanna C. Barry, Lindsey Christ, James W. Fourqurean, Thomas K. Frazer, Samantha T. Linhardt, Charles W. Martin, Ashley M. McDonald, Vivienne A. Main, Sarah A. Manuel, Candela Marco-Méndez, Laura K. Reynolds, Alex Rodriguez, Lucia M. Rodriguez Bravo, Yvonne Sawall, Khalil Smith, William L. Wied, Chang Jae Choi, and Ulrich Stingl

Subjects
Thalassia, seagrass microbiome, amplicon sequencing, Caribbean, seagrass beds, seagrass, Microbiology, QR1-502
Abstract

Plant microbiomes are known to serve several important functions for their host, and it is therefore important to understand their composition as well as the factors that may influence these microbial communities. The microbiome of Thalassia testudinum has only recently been explored, and studies to-date have primarily focused on characterizing the microbiome of plants in a single region. Here, we present the first characterization of the composition of the microbial communities of T. testudinum across a wide geographical range spanning three distinct regions with varying physicochemical conditions. We collected samples of leaves, roots, sediment, and water from six sites throughout the Atlantic Ocean, Caribbean Sea, and the Gulf of Mexico. We then analyzed these samples using 16S rRNA amplicon sequencing. We found that site and region can influence the microbial communities of T. testudinum, while maintaining a plant-associated core microbiome. A comprehensive comparison of available microbial community data from T. testudinum studies determined a core microbiome composed of 14 ASVs that consisted mostly of the family Rhodobacteraceae. The most abundant genera in the microbial communities included organisms with possible plant-beneficial functions, like plant-growth promoting taxa, disease suppressing taxa, and nitrogen fixers.

Published
2024
Full Text
View/download PDF

118. Mantenimiento, cuidado y reparación de arquitecturas comunitarias en conflicto: El desmontaje

Author

Candela Morado

Subjects
mantenimiento y cuidado, ecologías de reparación, vulnerabilidad material, deshacer arquitectura, conflictos urbanos, Drawing. Design. Illustration, NC1-1940
Abstract

Este artículo reflexiona etnográficamente sobre cómo se aborda y concibe la vulnerabilidad material en las prácticas de sostenimiento comunitario de arquitecturas en conflicto. Nos apoyaremos en las teorías de mantenimiento, cuidado y reparación, para complementarlas/matizarlas a través de los aprendizajes cultivados durante el proceso de respuesta ante la quema de una biblioteca comunitaria en la periferia sur de Bogotá. Las prácticas colectivas de sostenimiento desplegadas para hacerse cargo del devenir de la arquitectura amenazada nos ayudan a traer al frente (I) ecologías de prácticas y de agencia distribuida; (II) temporalidades alternativas y futuros no previstos; y (III) respuestas creativas y generadoras ante el daño o el conflicto; así como también (IV) métodos tentativos y (V) métodos de “apertura” (o des-cajanegrización). A través de una etnografía del proceso de desmontaje problematizaremos los ecosistemas sociomateriales necesarios para sostener vidas ante un “mundo roto”.

Published
2024

122. ll microbiota intestinale come fattore di rischio dello sviluppo di aGVHD gastrointestinale in pazienti pediatrici sottoposti a trapianto allogenico di cellule staminali ematopoietiche

Author

Zama, D., Biagi, E., Rampelli, S., Turroni, S., Brigidi, P., Consolandi, C., Severgnini, M., Landi, E., Bossu, G., Carella, M., Merli, P., Decembrino, N., Zecca, M., Cesaro, S., Faraci, M., Prete, A., Locatelli, F., Pession, A., Candela, M., and R. Masetti. I.

Subjects
complicanze intestinali, microbiota, trapianto, microbiota, complicanze intestinali, trapianto
Published
2018

132. Prosthetic Joint Infections Caused by Mycobacterium tuberculosis Complex—An ESGIAI–ESGMYC Multicenter, Retrospective Study and Literature Review

Author

Alvaro Auñon, Llanos Salar-Vidal, Ignacio Mahillo-Fernandez, Francisco Almeida, Pedro Pereira, Jaime Lora-Tamayo, Tristan Ferry, Sarah Souèges, Aurélien Dinh, Rosa Escudero, Candela Menéndez Fernández-Miranda, Alicia Rico, Nicolo Rossi, and Jaime Esteban

Subjects
tuberculosis, prosthetic joint infection, treatment, surgery, duration, outcome, Biology (General), QH301-705.5
Abstract

Purpose: While tuberculosis remains a significant global health concern, prosthetic joint infections (PJIs) caused by members of the Mycobacterium tuberculosis complex are exceptionally rare. Our objective is to perform a retrospective search of new cases of this disease and analyze all cases available in the literature of tuberculous PJIs, aiming to detect factors that may influence patient outcomes. Methods: The ESGIAI and ESGMYC study groups were used to collect information on non-published cases of tuberculous prosthetic joint infections (PJIs). Additionally, a literature review of all published cases of tuberculous PJIs was conducted. All identified cases in the retrospective study and in the literature review were merged and included in the statistical analysis, involving both univariate and multivariate analyses. Results: Fifteen previously unreported cases of tuberculous prosthetic joint infections (PJIs) from four countries were detailed. Among them, ten patients were female, with a median age of 76 years. The hip was affected in 13 cases. Seven patients experienced co-infection with another microorganism. Treatment approaches varied, with 13 patients undergoing implant removal, one treated with DAIR (debridement, antibiotics, and implant retention), and one case was treated with an unknown treatment method. All patients received antibiotic therapy and achieved a cure. The literature review that was conducted detected 155 published cases. Univariate analysis revealed a statistical significance for previous tuberculosis, joint, and no importance of surgery for cure. Conclusions: Tuberculous prosthetic joint infection (PJI) is a rare condition, typically presenting as a localized chronic infection. Antibiotic treatment is essential for the management of these patients, but neither surgical treatment nor duration of treatment seems to have importance in the outcome.

Published
2024
Full Text
View/download PDF

134. CTLA4 p.Thr17Ala (c.49A>G) polymorphism associates with inhibitor development in argentine patients with severe hemophilia A

Author

Marchione, Vanina Daniela, Radic, Claudia Pamela, Abelleyro, Miguel Martin, Primiani, L., Neme, D., Candela, M., de Tezanos Pinto, M., de Brasi, Carlos Daniel, and Rossetti, Liliana Carmen

Subjects
purl.org/becyt/ford/1 [https], Ciencias Biológicas, Ctla4, Inhibidores-Fviii, Otros Tópicos Biológicos, purl.org/becyt/ford/1.6 [https], F8, Hema, CIENCIAS NATURALES Y EXACTAS
Abstract

El desarrollo de inhibidores de FVIII en hemofilia A (HA) es considerado un rasgo complejo, ya que involucra factores genéticos y ambientales, siendo el genotipo del gen del factor VIII (F8) el factor condicionante más importante, seguido por factores genéticos secundarios, más débiles. Se estimaron los riesgos de inhibidor asociados a cada genotipo-F8 mediante un estudio de casos/ controles en pacientes HA-severos (n=390), que caracteriza especialmente el estrato con la Inv22 (inversión del intrón 22). El cálculo de la prevalencia de inhibidor (IP) y odds-ratio (OR) con intervalos de confianza del 95% (IC95%) permitió clasificar tres grupos de riesgo (alto, medio y bajo) asociado a cada genotipo-F8. La asociación de factores genéticos secundarios se investigó mediante el análisis de concordancia/discordancia en el estatus de inhibidor en 17 pares de hermanos con la Inv22 vs pares al azar mostrando un OR(IC95%) de 1,83(0,69-4,85) (p=0,33), sugiriendo una tendencia a coincidir con el estatus de inhibidor del hermano. Se realizaron estudios tipo caso/control del riesgo de inhibidor en polimorfismos de IL10, TNFA y CTLA4 en los estratos Inv22-positivo (n=140-148). IL10 c.- 1117A>G, TNFA c.-488G>A y CTLA4 c.-319C>T mostraron tendencias de riesgo o protección similares a las reportadas, con ORs no significativos. CTLA4 c.49A>G p.Thr17Ala mostró un incremento significativo del riesgo de inhibidor con OR de 2,61(1,27-5,36) (p=0,0096). Nuestros resultados concuerdan con especulaciones teóricas previas acerca de diferencias regionales en los factores secundarios no modificables. CTLA4 p.Thr17Ala contribuye a aumentar el riesgo de inhibidor en nuestra población de pacientes con HA-severa. FVIII inhibitor development in hemophilia A (HA) is considered a complex trait as it involves genetic and environmental factors; the causative factor VIII gene (F8) genotype has been established as the most important determining factor, followed by weaker secondary genetic risks factors. Risks of inhibitor development associated with each F8- genotype were estimated by a case/control study in HA-severe patients (n=390), which especially characterizes strata with Inv22 (intron 22 inversion). Inhibitor prevalence (IP) and odds ratio (OR) with confidence intervals of 95% (95%CI) calculations allowed classifying three risk groups (high, medium and low) associated with each F8-genotype. The association of genetic factors was investigated by analyzing concordance/discordance inhibitor-status in 17 pairs of brothers with Inv22 vs random pairs showing 1.83(0.69 to 4.85) (p=0.33), suggesting a trend to agree the inhibitor status between siblings. Case/control studies associated risk inhibitor development with IL10, TNFA and CTLA4 polymorphisms in Inv22-positive strata (n=140- 148) were performed and in IL10 c.-1117A>G, TNFA c.-488G>A & CTLA4 c.-319C>T trends of risks or protection, similar to reported ones with not significant ORs. CTLA4 c.49A>G p.Thr17Ala showed significantly increased inhibitor risks with OR of 2.61(1.27-5.36) (p=0.0096). Our findings agree with previous theoretical speculations about regional differences in non-modifiable secondary factors. CTLA4 p.Thr17Ala, contributes to an increased risk of inhibitor in our population of patients with HA-sever Fil: Marchione, Vanina Daniela. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Medicina Experimental. Academia Nacional de Medicina de Buenos Aires. Instituto de Medicina Experimental; Argentina Fil: Radic, Claudia Pamela. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Medicina Experimental. Academia Nacional de Medicina de Buenos Aires. Instituto de Medicina Experimental; Argentina Fil: Abelleyro, Miguel Martin. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Medicina Experimental. Academia Nacional de Medicina de Buenos Aires. Instituto de Medicina Experimental; Argentina Fil: Primiani, L.. Fundación de la Hemofilia Dr. Alfredo Pavlovsky; Argentina Fil: Neme, D.. Fundación de la Hemofilia Dr. Alfredo Pavlovsky; Argentina Fil: Candela, M.. Fundación de la Hemofilia Dr. Alfredo Pavlovsky; Argentina Fil: de Tezanos Pinto, M.. Academia Nacional de Medicina de Buenos Aires. Instituto de Investigaciones Hematológicas "Mariano R. Castex". Departamento de Genética; Argentina. Fundación de la Hemofilia Dr. Alfredo Pavlovsky; Argentina Fil: de Brasi, Carlos Daniel. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Medicina Experimental. Academia Nacional de Medicina de Buenos Aires. Instituto de Medicina Experimental; Argentina. Academia Nacional de Medicina de Buenos Aires. Instituto de Investigaciones Hematológicas "Mariano R. Castex". Departamento de Genética; Argentina Fil: Rossetti, Liliana Carmen. Consejo Nacional de Investigaciones Científicas y Técnicas. Instituto de Medicina Experimental. Academia Nacional de Medicina de Buenos Aires. Instituto de Medicina Experimental; Argentina

Published
2016

143. Unraveling the gut microbiome of the long-lived naked mole-rat.

Author

Debebe, T, Biagi, E, Soverini, M, Holtze, S, Hildebrandt, TB, Birkemeyer, C, Wyohannis, D, Lemma, A, Brigidi, P, Savkovic, V, König, B, Candela, M, Birkenmeier, G, Debebe, T, Biagi, E, Soverini, M, Holtze, S, Hildebrandt, TB, Birkemeyer, C, Wyohannis, D, Lemma, A, Brigidi, P, Savkovic, V, König, B, Candela, M, and Birkenmeier, G

Abstract

The naked mole-rat (Heterocephalus glaber) is a subterranean mouse-sized African mammal that shows astonishingly few age-related degenerative changes and seems to not be affected by cancer. These features make this wild rodent an excellent model to study the biology of healthy aging and longevity. Here we characterize for the first time the intestinal microbial ecosystem of the naked mole-rat in comparison to humans and other mammals, highlighting peculiarities related to the specific living environment, such as the enrichment in bacteria able to utilize soil sulfate as a terminal electron acceptor to sustain an anaerobic oxidative metabolism. Interestingly, some compositional gut microbiota peculiarities were also shared with human gut microbial ecosystems of centenarians and Hadza hunter-gatherers, considered as models of a healthy gut microbiome and of a homeostatic and highly adaptive gut microbiota-host relationship, respectively. In addition, we found an enrichment of short-chain fatty acids and carbohydrate degradation products in naked mole-rat compared to human samples. These data confirm the importance of the gut microbial ecosystem as an adaptive partner for the mammalian biology and health, independently of the host phylogeny.

Published
2017

145. The bottlenose dolphin (Tursiops truncatus) fecal microbiota

Author

Soverini M, Quercia S, Biancani B, Furlati S, Turroni S, Biagi E, Consolandi C, Peano C, Severgnini M, Rampelli S, Brigidi P, and Candela M.

Subjects
digestive system, 16S rDNA, Tursiops truncatus, cetacea, evolution, fecal microbiota, mammalia
Abstract

Cetaceans have evolved from herbivorous terrestrial artiodactyls closely related to ruminants and hippopotamuses. Delphinidae, a family included in this order, represent an extreme and successful re-adaptation of mammalian physiology to the marine habitat and piscivorous diet. The anatomical aspects of Delphinidae success are well understood, whereas some physiological aspects of their environmental fitness are less defined, such as the gut microbiota composition and its adaptation to their dietary niche. Here, we explored the fecal microbiota structure of nine adult bottlenose dolphins (Tursiops truncatus) and one breast-fed calf living in a controlled environment. According to our findings, dolphins possess a unique microbiota profile within the Mammalia class, highly resembling that of carnivorous marine fishes. The breast-fed calf showed a distinctive compositional structure of the gut microbial ecosystem, which partially overlaps with the mother's milk microbiota. Taken together, our data indicate that in dolphins the adaptation to the marine niche and piscivorous diet involved the convergence of their gut microbiota structure with that of marine fishes, overcoming the gut microbiota phylogenetic inertia previously described in terrestrial mammalians.

Published
2016

146. The Typhoid Toxin Promotes Host Survival and the Establishment of a Persistent Asymptomatic Infection

Author

Del Bel Belluz, L. Guidi, R. Pateras, I.S. Levi, L. Mihaljevic, B. Rouf, S.F. Wrande, M. Candela, M. Turroni, S. Nastasi, C. Consolandi, C. Peano, C. Tebaldi, T. Viero, G. Gorgoulis, V.G. Krejsgaard, T. Rhen, M. Frisan, T.

Abstract

Bacterial genotoxins, produced by several Gram-negative bacteria, induce DNA damage in the target cells. While the responses induced in the host cells have been extensively studied in vitro, the role of these effectors during the course of infection remains poorly characterized. To address this issue, we assessed the effects of the Salmonella enterica genotoxin, known as typhoid toxin, in in vivo models of murine infection. Immunocompetent mice were infected with isogenic S. enterica, serovar Typhimurium (S. Typhimurium) strains, encoding either a functional or an inactive typhoid toxin. The presence of the genotoxic subunit was detected 10 days post-infection in the liver of infected mice. Unexpectedly, its expression promoted the survival of the host, and was associated with a significant reduction of severe enteritis in the early phases of infection. Immunohistochemical and transcriptomic analysis confirmed the toxin-mediated suppression of the intestinal inflammatory response. The presence of a functional typhoid toxin further induced an increased frequency of asymptomatic carriers. Our data indicate that the typhoid toxin DNA damaging activity increases host survival and favours long-term colonization, highlighting a complex cross-talk between infection, DNA damage response and host immune response. These findings may contribute to understand why such effectors have been evolutionary conserved and horizontally transferred among Gram-negative bacteria. © 2016 Del Bel Belluz et al.

Published
2016

147. Metagenomic shifts in mucus, tissue and skeleton of the coral Balanophyllia europaea living along a natural CO2 gradient

Author

Palladino Giorgia, Caroselli Erik, Tavella Teresa, Federica D’Amico, Prada Fiorella, Mancuso Arianna, Franzellitti Silvia, Rampelli Simone, Candela Marco, Goffredo Stefano, and Biagi Elena

Subjects
Microbial ecology, QR100-130
Abstract

Abstract Using the Mediterranean coral Balanophyllia europaea naturally growing along a pH gradient close to Panarea island (Italy) as a model, we explored the role of host-associated microbiomes in coral acclimatization to ocean acidification (OA). Coral samples were collected at three sites along the gradient, mimicking seawater conditions projected for 2100 under different IPCC (The Intergovernmental Panel on Climate Change) scenarios, and mucus, soft tissue and skeleton associated microbiomes were characterized by shotgun metagenomics. According to our findings, OA induced functional changes in the microbiomes genetic potential that could mitigate the sub-optimal environmental conditions at three levels: i. selection of bacteria genetically equipped with functions related to stress resistance; ii. shifts in microbial carbohydrate metabolism from energy production to maintenance of cell membranes and walls integrity; iii. gain of functions able to respond to variations in nitrogen needs at the holobiont level, such as genes devoted to organic nitrogen mobilization. We hence provided hypotheses about the functional role of the coral associated microbiome in favoring host acclimatation to OA, remarking on the importance of considering the crosstalk among all the components of the holobiont to unveil how and to what extent corals will maintain their functionality under forthcoming ocean conditions.

Published
2022
Full Text
View/download PDF

149. Evaluation of Combination Drug Therapy for Treatment of Antibiotic-Resistant Inhalation Anthrax in a Murine Model

Author

Heine, H. S., primary, Shadomy, S. V., additional, Boyer, A. E., additional, Chuvala, L., additional, Riggins, R., additional, Kesterson, A., additional, Myrick, J., additional, Craig, J., additional, Candela, M. G., additional, Barr, J. R., additional, Hendricks, K., additional, Bower, W. A., additional, Walke, H., additional, and Drusano, G. L., additional

Published
2017
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results