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2. The global response to the COVID-19 pandemic: how have immunology societies contributed?

Author

Osier, Faith, Ting, Jenny, Fraser, John, Lambrecht, Bart, Romano, Marta, Gazzinelli, Ricardo, Bortoluci, Karina, Zamboni, Dario, Akbar, Arne, Evans, Jennie, Brown, Doug, Patel, Kamala, Wu, Yuzhang, Perez, Ana, Pérez, Oliver, Kamradt, Thomas, Falk, Christine, Barda-Saad, Mira, Ariel, Amiram, Santoni, Angela, Annunziato, Francesco, Cassatella, Marco, Kiyono, Hiroshi, Chereshnev, Valeriy, Dieye, Alioune, Mbow, Moustapha, Mbengue, Babacar, Niang, Maguette, and Suchard, Melinda

Subjects
Antiviral Agents, Betacoronavirus, COVID-19, COVID-19 Vaccines, Community-Institutional Relations, Coronavirus Infections, Global Health, Humans, International Cooperation, Pandemics, Patient Education as Topic, Personal Protective Equipment, Pneumonia, Viral, SARS-CoV-2, Severe Acute Respiratory Syndrome, Societies, Scientific, Viral Vaccines
Abstract

The COVID-19 pandemic is shining a spotlight on the field of immunology like never before. To appreciate the diverse ways in which immunologists have contributed, Nature Reviews Immunology invited the president of the International Union of Immunological Societies and the presidents of 15 other national immunology societies to discuss how they and their members responded following the emergence of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2).

Published
2020

5. Intranasal dexamethasone: a new clinical trial for the control of inflammation and neuroinflammation in COVID-19 patients

Author

Cárdenas, Graciela, Chávez-Canales, María, Espinosa, Ana María, Jordán-Ríos, Antonio, Malagon, Daniel Anica, Murillo, Manlio Fabio Márquez, Araujo, Laura Victoria Torres, Campos, Ricardo Leopoldo Barajas, Wong-Chew, Rosa María, González, Luis Esteban Ramirez, Cresencio, Karent Ibet, Velázquez, Enrique García, de la Cerda, Mariana Rodriguez, Leyva, Yoana, Hernández-Ruiz, Joselin, Hernández-Medel, María Luisa, León-Hernández, Mireya, Quero, Karen Medina, Monciváis, Anahí Sánchez, Díaz, Sergio Hernández, Martínez, Ignacia Rosalia Zeron, Martínez-Cuazitl, Adriana, Salazar, Iván Noé Martínez, Sarmiento, Eduardo Beltrán, Peña, Aldo Figueroa, Hernández, Patricia Saraí, Reynoso, Rafel Ignacio Aguilar, Reyes, Daniela Murillo, del Río Ambriz, Luis Rodrigo, Bonilla, Rogelio Antonio Alfaro, Cruz, Jocelyn, Huerta, Leonor, Fierro, Nora Alma, Hernández, Marisela, Pérez-Tapia, Mayra, Meneses, Gabriela, Espíndola-Arriaga, Erick, Rosas, Gabriela, Chinney, Alberto, Mendoza, Sergio Rosales, Hernández-Aceves, Juan Alberto, Cervantes-Torres, Jaquelynne, Rodríguez, Anai Fuentes, Alor, Roxana Olguin, Francisco, Sandra Ortega, Salazar, Evelyn Alvarez, Besedovsky, Hugo, Romano, Marta C., Bobes, Raúl J., Jung, Helgi, Soldevila, Gloria, López-Alvarenga, Juan, Fragoso, Gladis, Laclette, Juan Pedro, and Sciutto, Edda

Published
2022
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8. A randomized, multicentre, open-label phase II proof-of-concept trial investigating the clinical efficacy and safety of the addition of convalescent plasma to the standard of care in patients hospitalized with COVID-19: the Donated Antibodies Working against nCoV (DAWn-Plasma) trial

Author

Devos, Timothy, Geukens, Tatjana, Schauwvlieghe, Alexander, Ariën, Kevin K., Barbezange, Cyril, Cleeren, Myriam, Compernolle, Veerle, Dauby, Nicolas, Desmecht, Daniël, Grimaldi, David, Lambrecht, Bart N., Luyten, Anne, Maes, Piet, Moutschen, Michel, Romano, Marta, Seyler, Lucie, Nevessignsky, Michel Toungouz, Vandenberghe, Katleen, van Griensven, Johan, Verbeke, Geert, Vlieghe, Erika, Yombi, Jean Cyr, Liesenborghs, Laurens, Verhamme, Peter, and Meyfroidt, Geert

Published
2020
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9. Correction to: A randomized, multicentre, open-label phase II proof-of-concept trial investigating the clinical efficacy and safety of the addition of convalescent plasma to the standard of care in patients hospitalized with COVID-19: the Donated Antibodies Working against nCoV (DAWn-Plasma) trial

Author

Devos, Timothy, Geukens, Tatjana, Schauwvlieghe, Alexander, Ariën, Kevin K., Barbezange, Cyril, Cleeren, Myriam, Compernolle, Veerle, Dauby, Nicolas, Desmecht, Daniël, Grimaldi, David, Lambrecht, Bart N., Luyten, Anne, Maes, Piet, Moutschen, Michel, Romano, Marta, Seyler, Lucie, Nevessignsky, Michel Toungouz, Vandenberghe, Katleen, van Griensven, Johan, Verbeke, Geert, Vlieghe, Erika, Yombi, Jean Cyr, Liesenborghs, Laurens, Verhamme, Peter, and Meyfroidt, Geert

Published
2020
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10. Low responsiveness of peripheral lymphocytes in extraparenchymal neurocysticercosis.

Author

Romo, Matthew L., Osorio, Rocio, Toledo, Andrea, Carrillo-Mezo, Roger, Valdez, Ricardo, Romano, Marta C., Sciutto, Edda, Fragoso, Gladis, and Fleury, Agnès

Subjects
CENTRAL nervous system infections, NEUROCYSTICERCOSIS, ESTRADIOL, KILLER cells, LYMPHOCYTES, TAENIA solium
Abstract

Background: The morbidity and mortality of extraparenchymal neurocysticercosis (EP-NC) remain high and effectiveness of current medical treatment is suboptimal. Various factors have been implicated in the severity of EP-NC and in the poor response to treatment, but the possible role of host immune and endocrine systems has not yet been examined thoroughly. Methodology/Principal findings: 42 participants with EP-NC before receiving standard treatment and 25 healthy controls were included in the study. Treatment response was assessed by comparing pre/post treatment parasite volumes from 3D MRI. Prior to treatment among participants with EP-NC, specific stimulation induced an increased specific proliferative response accompanied by a significant increase in IL-4, NK, NKT, Bregs and Tregs cells, whereas in healthy controls, specific stimulation induced a significant increase in IL-1β, IL-5, CCL5, IL-6, TNF-α, NK and Bregs cells. Significant differences between participants with EP-NC and healthy controls in the specific inflammatory response were observed. Participants with EP-NC prior to treatment had significantly weaker responses of proinflammatory cytokines (IL-6, TNF-α) and NK cells, and stronger IL-4 response. Anthelmintic treatment did not promote significant peripheral immunological changes at any time, although inflammation was sustained in the cerebrospinal fluid. Serum estradiol concentration significantly decreased after anthelmintic treatment among males, and cortisol correlated negatively with IL-6 and positively with IFN-γ levels. No pre-treatment immunologic or endocrinologic parameters were significantly associated with response to treatment. Conclusion/Significance: Prior to anthelmintic treatment, EP-NC was characterized by low lymphocyte reactivity accompanied by a regulatory response, which may be involved in the lack of peripheral immunological changes during and after treatment, although a central inflammatory response was present. This weak specific peripheral response could favor the chronicity of the infection and the poor response to treatment. Our findings highlight the need for new anti-inflammatory treatment focused on the central nervous system with less systemic immunosuppressive effects. Author summary: Neurocysticercosis is a central nervous system infection with the helminth Taenia solium in its larval stage. It is a marker of poverty and remains endemic in countries of Latin America, Africa, and Asia. The severity of neurocysticercosis and the prognosis of patients depend on the location of the parasites. Extraparenchymal infection involving the subarachnoid and/or ventricular space is associated with high morbidity and mortality and a suboptimal response to current anthelminthic treatment regimens. We examined peripheral immunological parameters and hormones of 42 participants with extraparenchymal neurocysticercosis before and after treatment, and their associations with subsequent treatment response. Prior to treatment, compared with healthy controls, there was low lymphocyte reactivity with a regulatory response, which may explain the lack of peripheral immunological changes during and after treatment. This weak specific peripheral response could favor the chronicity of the infection and the poor response to treatment and should be considered in research to improve patient outcomes. [ABSTRACT FROM AUTHOR]

Published
2023
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13. Liver X receptors contribute to the protective immune response against Mycobacterium tuberculosis in mice

Author

Korf, Hannelie, Beken, Seppe Vander, Romano, Marta, Steffensen, Knut R., Stijlemans, Benoit, Gustafsson, Jan-Ake, Grooten, Johan, and Huygen, Kris

Subjects
Cell receptors -- Physiological aspects, Cell receptors -- Research, Mice -- Usage, Mice -- Models, Immune response -- Health aspects, Immune response -- Research, Mycobacterium tuberculosis -- Health aspects, Mycobacterium tuberculosis -- Research
Abstract

Liver X receptors (LXRs) are key regulators of macrophage function, controlling transcriptional programs involved in lipid homeostasis and inflammation. However, exactly how LXRs modulate inflammation during infection remains unknown. To explore this, we used a mouse model of Mycobacterium tuberculosis infection. Upon intratracheal infection with M. tuberculosis, LXRs and LXR target genes were induced in [CD11c.sup.+] lung and alveolar cells. Furthermore, mice deficient in both LXR isoforms, LXR[alpha] and LXR[beta] (Lxra-/-Lxrb-/- mice), were more susceptible to infection, developing higher bacterial burdens and an increase in the size and number of granulomatous lesions. Interestingly, mice solely deficient in LXR[alpha], but not those lacking only LXR[beta], mirrored the susceptibility of the Lxra-/-Lxrb-/- animals. Lxra-/-Lxrb-/- mice failed to mount an effective early neutrophilic airway response to infection and showed dysregulation of both pro- and antiinflammatory factors in [CD11c.sup.+] lung cells. T cell responses were strongly affected in Lxra-/-Lxrb-/- mice, showing near-complete abrogation of the infection-induced Th1 function--and even more so Th17 function--in the lungs. Treatment of WT mice with the LXR agonists TO901317 and GW3965 resulted in a 10-fold decrease of the pulmonary bacterial burden and a comparable increase of Th1/Th17 function in the lungs. The dependence of LXR signaling on the neutrophil IL-17 axis represents what we believe to be a novel function for these nuclear receptors in resistance to M. tuberculosis infection and may provide a new target for therapeutics., Introduction An estimated one-third of the world population is latently infected with Mycobacterium tuberculosis (1), creating a vast reservoir from which most active cases of tuberculosis arise. The success of [...]

Published
2009

14. SARS-CoV-2 neutralising antibody testing in Europe: towards harmonisation of neutralising antibody titres for better use of convalescent plasma and comparability of trial data.

Author

Dung Nguyen, Simmonds, Peter, Steenhuis, Maurice, Wouters, Elise, Desmecht, Daniel, Garigliany, Mutien, Romano, Marta, Barbezange, Cyril, Maes, Piet, Van Holm, Bram, Mendoza, Joaquín, Oyonarte, Salvador, Fomsgaard, Anders, Lassaunière, Ria, Zusinaite, Eva, Rus, Katarina Resman, Avšič-Županc, Tatjana, Reimerink, Johan H. J., Brouwer, Fiona, and Hoogerwerf, Marieke

Published
2021
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17. Glioblastoma cells express crucial enzymes involved in androgen synthesis: 3β‐hydroxysteroid dehydrogenase, 17‐20α‐hydroxylase, 17β‐hydroxysteroid dehydrogenase and 5α‐reductase.

Author

Mondragón, Jose Antonio, Serrano, Yesenia, Torres, Andrea, Orozco, Martin, Segovia, Jose, Manjarrez, Gabriel, and Romano, Marta Catalina

Subjects
GLIOBLASTOMA multiforme, ANDROGENS, STEROIDS
Abstract

Glioblastoma (GB) is the most common and aggressive primary brain tumour in adult humans. Therapeutic resistance and tumour recurrence after surgical removal contribute to poor prognosis for glioblastoma patients. Men are known to be more likely than women to develop an aggressive form of GB, and differences in sex steroids have emerged as a leading explanation for this finding. Studies indicate that the metabolism and proliferation of GB‐derived cells are increased by sex steroids, the expression of androgen receptors (ARs) and the synthesis of androgens and oestrogens, suggesting that these hormones have a role in the tumour pathogenesis. The expression of aromatase, the enzyme that converts androgens to oestrogens, has been reported in glial cells and GB cell lines. Thus, it was necessary to test whether the steroidogenic enzymes involved in androgen synthesis are expressed in GB cells. Therefore, here, we investigated the expression of four key enzymes involved in androgen synthesis in human‐derived GB cells. U87 cells were cultured in Dulbecco's modified Eagle medium plus foetal bovine serum and antibiotics on slides for immunocytochemistry or immunofluorescence. U87, LN229 and C6 cells were also cultured in multi‐well chambers to obtain proteins for Western blotting. We used primary antibodies against 3β‐hydroxysteroid dehydrogenase (3β‐HSD), 17α‐hydroxilase/17,20‐lyase (P450c17), 17β‐hydroxysteroid dehydrogenase (17β‐HSD) and 5α‐reductase. Immunocytochemistry, and immunofluorescence results revealed that glioblastoma cells express 3β‐HSD, P450c17, 17β‐HSD and 5α‐reductase proteins in their cytoplasm. Moreover, Western blot analyses revealed bands corresponding to the molecular weight of these four enzymes in the three GB cell lines. Thus, glioblastoma cells have the key enzymatic machinery necessary to synthesize androgens, and these enzymes might be useful targets for new therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published
2021
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18. DNA damage and health effects in juvenile haddock (Melanogrammus aeglefinus) exposed to PAHs associated with oil-polluted sediment or produced water.

Author

Meier, Sonnich, Karlsen, Ørjan, Le Goff, Jeremie, Sørensen, Lisbet, Sørhus, Elin, Pampanin, Daniela M., Donald, Carey E., Fjelldal, Per Gunnar, Dunaevskaya, Evgenia, Romano, Marta, Caliani, Ilaria, Casini, Silvia, Bogevik, André S., Olsvik, Pål A., Myers, Mark, and Grøsvik, Bjørn Einar

Subjects
OIL field brines, DNA adducts, POLYCYCLIC aromatic hydrocarbons, DRILLING muds, HEAVY oil, PETROLEUM, DNA damage
Abstract

The research objective was to study the presence of DNA damages in haddock exposed to petrogenic or pyrogenic polyaromatic hydrocarbons (PAHs) from different sources: 1) extracts of oil produced water (PW), dominated by 2-ring PAHs; 2) distillation fractions of crude oil (representing oil-based drilling mud), dominated by 3-ring PAHs; 3) heavy pyrogenic PAHs, mixture of 4/5/6-ring PAHs. The biological effect of the different PAH sources was studied by feeding juvenile haddock with low doses of PAHs (0.3–0.7 mg PAH/kg fish/day) for two months, followed by a two-months recovery. In addition to the oral exposure, a group of fish was exposed to 12 single compounds of PAHs (4/5/6-ring) via intraperitoneal injection. The main endpoint was the analysis of hepatic and intestinal DNA adducts. In addition, PAH burden in liver, bile metabolites, gene and protein expression of CYP1A, GST activity, lipid peroxidation, skeletal deformities and histopathology of livers were evaluated. Juvenile haddock responded quickly to both intraperitoneal injection and oral exposure of 4/5/6-ring PAHs. High levels of DNA adducts were detected in livers three days after the dose of the single compound exposure. Fish had also high levels of DNA adducts in liver after being fed with extracts dominated by 2-ring PAHs (a PW exposure scenario) and 3-ring PAHs (simulating an oil exposure scenario). Elevated levels of DNA adducts were observed in the liver of all exposed groups after the 2 months of recovery. High levels of DNA adduct were found also in the intestines of individuals exposed to oil or heavy PAHs, but not in the PW or control groups. This suggests that the intestinal barrier is very important for detoxification of orally exposures of PAHs. [ABSTRACT FROM AUTHOR]

Published
2020
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19. In cooperation with Anesthesia Case of the Month.

Author

Garbin, Marta, Romano, Marta, Stern, Adam W., and Iredale, Marley E.

Subjects
*ACID-base imbalances, *PERSPIRATION, *ENDOTOXINS, *ARRHYTHMIA, *THOROUGHBRED horse, *ANESTHESIA, *HORSE diseases
Abstract

The article presents a case study of An 18-year-old American Quarter Horse mare was referred to the University of Florida Large Animal Hospital because of signs of colic for > 7 hours. The referring veterinarian treated the mare with flunixin meglumine about 6 hours before the referral examination. Abdominal ultrasonography revealed gas distention of the large colon. A complete rectal examination was prevented by the presence of the gas-distended large colon in the pelvic canal.

Published
2020
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20. A retrospective analysis of the epidural use of bupivacaine 0.0625-0.125% with opioids in bitches undergoing cesarean section.

Author

Martin-Flores, Manuel, Anderson, Justine C., Sakai, Daniel M., Campoy, Luis, Soon Hon Cheong, Romano, Marta, and Gleed, Robin D.

Subjects
CESAREAN section, FENTANYL, LOCAL anesthetics, RETROSPECTIVE studies, EPIDURAL anesthesia, GENERAL anesthesia
Abstract

Copyright of Canadian Veterinary Journal / Revue Vétérinaire Canadienne is the property of Canadian Veterinary Medical Association and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2019

21. INFLUENCIA DE LA TESTOSTERONA SOBRE LA INFECCIÓN CAUSADA POR TRYPANOSOMA CRUZI.

Author

PÉREZ, ANA ROSA, PASCUTTI, MARÍA FERNANDA, FONTANELLA, GERMÁN H., MARTÍN, ANA P., TARTALINI, VANINA, NOCITO, ANA LÍA, BERRA, HÉCTOR H., PEZZOTTO, STELLA M., ROMANO, MARTA C., and REVELLI, SILVIA S.

Abstract

Copyright of Revista Médica de Rosario is the property of Circulo Medico de Rosario and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2019

22. Allergic Asthma Favors Brucella Growth in the Lungs of Infected Mice.

Author

Machelart, Arnaud, Potemberg, Georges, Van Maele, Laurye, Demars, Aurore, Lagneaux, Maxime, De Trez, Carl, Sabatel, Catherine, Bureau, Fabrice, De Prins, Sofie, Percier, Pauline, Denis, Olivier, Jurion, Fabienne, Romano, Marta, Vanderwinden, Jean-Marie, Letesson, Jean-Jacques, and Muraille, Eric

Subjects
ASTHMA -- Immunological aspects, LUNG diseases, BRUCELLA
Abstract

Allergic asthma is a chronic Th2 inflammatory disease of the lower airways affecting a growing number of people worldwide. The impact of infections and microbiota composition on allergic asthma has been investigated frequently. Until now, however, there have been few attempts to investigate the impact of asthma on the control of infectious microorganisms and the underlying mechanisms. In this work, we characterize the consequences of allergic asthma on intranasal (i.n.) infection by Brucella bacteria in mice. We observed that i.n. sensitization with extracts of the house dust mite Dermatophagoides farinae or the mold Alternaria alternata (Alt) significantly increased the number of Brucella melitensis, Brucella suis , and Brucella abortus in the lungs of infected mice. Microscopic analysis showed dense aggregates of infected cells composed mainly of alveolar macrophages (CD11c+ F4/80+ MHCII+) surrounded by neutrophils (Ly-6G+). Asthma-induced Brucella susceptibility appears to be dependent on CD4+ T cells, the IL-4/STAT6 signaling pathway and IL-10, and is maintained in IL-12- and IFN-γR-deficient mice. The effects of the Alt sensitization protocol were also tested on Streptococcus pneumoniae and Mycobacterium tuberculosis pulmonary infections. Surprisingly, we observed that Alt sensitization strongly increases the survival of S. pneumoniae infected mice by a T cell and STAT6 independent signaling pathway. In contrast, the course of M. tuberculosis infection is not affected in the lungs of sensitized mice. Our work demonstrates that the impact of the same allergic sensitization protocol can be neutral, negative, or positive with regard to the resistance of mice to bacterial infection, depending on the bacterial species. [ABSTRACT FROM AUTHOR]

Published
2018
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23. Differential Susceptibility to infectious Respiratory Diseases between Males and Females Linked to Sex-Specific innate immune inflammatory Response.

Author

Chamekh, Mustapha, Deny, Maud, Romano, Marta, Lefèvre, Nicolas, Corazza, Francis, Duchateau, Jean, and Casimir, Georges

Subjects
RESPIRATORY disease diagnosis, NATURAL immunity, DISEASE susceptibility
Abstract

It is widely acknowledged that males and females exhibit contrasting degrees of susceptibility to infectious and non-infectious inflammatory diseases. This is particularly observed in respiratory diseases where human males are more likely to be affected by infection-induced acute inflammations compared to females. The type and magnitude of the innate immune inflammatory response play a cardinal role in this sex bias. Animal models mimicking human respiratory diseases have been used to address the biological factors that could explain the distinct outcomes. In this review, we focus on our current knowledge about experimental studies investigating sex-specific differences in infection-induced respiratory diseases and we provide an update on the most important innate immune mechanisms that could explain sex bias of the inflammatory response. We also discuss whether conclusions drawn from animal studies could be relevant to human. [ABSTRACT FROM AUTHOR]

Published
2017
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24. Trypanosoma Infection Favors Brucella Elimination via IL-12/IFNγ- Dependent Pathways.

Author

Machelart, Arnaud, Van Vyve, Margaux, Potemberg, Georges, Demars, Aurore, De Trez, Carl, Tima, Hermann Giresse, Vanwalleghem, Gilles, Romano, Marta, Truyens, Carine, Letesson, Jean-Jacques, and Muraille, Eric

Subjects
TRYPANOSOMATIDAE, ETIOLOGY of diseases
Abstract

This study develops an original co-infection model in mice using Brucella melitensis, the most frequent cause of human brucellosis, and Trypanosoma brucei, the agent of African trypanosomiasis. Although the immunosuppressive effects of T. brucei in natural hosts and mice models are well established, we observed that the injection of T. brucei in mice chronically infected with B. melitensis induces a drastic reduction in the number of B. melitensis in the spleen, the main reservoir of the infection. Similar results are obtained with Brucella abortus-and Brucella suis-infected mice and B. melitensis-infected mice co-infected with Trypanosoma cruzi, demonstrating that this phenomenon is not due to antigenic cross-reactivity. Comparison of co-infected wild-type and genetically deficient mice showed that Brucella elimination required functional IL-12p35/IFNγ signaling pathways and the presence of CD4+ T cells. However, the impact of wild type and an attenuated mutant of T. brucei on B. melitensis were similar, suggesting that a chronic intense inflammatory reaction is not required to eliminate B. melitensis. Finally, we also tested the impact of T. brucei infection on the course of Mycobacterium tuberculosis infection. Although T. brucei strongly increases the frequency of IFNγ+CD4+ T cells, it does not ameliorate the control of M. tuberculosis infection, suggesting that it is not controlled by the same effector mechanisms as Brucella. Thus, whereas T. brucei infections are commonly viewed as immunosuppressive and pathogenic, our data suggest that these parasites can specifically affect the immune control of Brucella infection, with benefits for the host. [ABSTRACT FROM AUTHOR]

Published
2017
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25. Inflammatory Properties and Adjuvant Potential of Synthetic Glycolipids Homologous to Mycolate Esters of the Cell Wall of Mycobacterium tuberculosis.

Author

Tima, Hermann Giresse, al Dulayymi, Juma''a Raheem, Denis, Olivier, Lehebel, Pauline, Baols, Klarah Sherzad, Mohammed, Mohsin Omar, L'Homme, Laurent, Sahb, Mohaned Mohammed, Potemberg, Georges, Legrand, Sylvie, Lang, Roland, Beyaert, Rudi, Piette, Jacques, Baird, Mark Stephen, Huygen, Kris, and Romano, Marta

Published
2017
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26. Proximal and Distal Predictors of the Spider Monkey’s Stress Levels in Fragmented Landscapes.

Author

Ordóñez-Gómez, José D., Cristóbal-Azkarate, Jurgi, Arroyo-Rodríguez, Víctor, Santillán-Doherty, Ana M., Valdez, Ricardo A., and Romano, Marta C.

Subjects
SPIDER monkeys, PHYSIOLOGICAL stress, FOREST management, LANDSCAPE protection, BIODEGRADATION, ANIMAL species, ANIMAL health
Abstract

The rapid loss, fragmentation and degradation of tropical forests threaten the survival of many animal species. However, the way in which these phenomena affect animal health has been poorly explored, thus limiting the design of appropriate conservation strategies. To address this, here we identified using linear mixed models the effect of proximal (diet, activity pattern, hunting and logging) and distal (sum of the basal areas of fruiting-tree species [SBAFS], landscape forest cover and degree of forest fragmentation) variables over fecal glucocorticoid metabolite (fGCM) levels–hormones associated with animal health and fitness–of six groups of spider monkeys (Ateles geoffroyi) inhabiting six landscapes with different spatial structures in Mexico. Proximal variables showed a stronger predictive power over fGCMs than distal. In this sense, increases in travel time, the occurrence of hunting, and reductions in rest time and fruit consumption resulted in higher fGCM levels. Regarding distal variables, increases in SBAFS were negatively related to fGCM levels, thus suggesting that food scarcity increases stress hormone levels. Nevertheless, contrary to theoretical expectations, spider monkeys living in smaller tracts of forest spent less time travelling, but the same time feeding on fruit as those in more forested areas. The lower net energy return associated with this combination of factors would explain why, contrary to theoretical expectations, increased forest cover was associated with increased levels of fGCMs in these groups. Our study shows that, at least in the short term, spider monkeys in fragmented landscapes do not always present higher levels of stress hormones compared to those inhabiting continuous forest, and the importance of preserving fruit sources and controlling hunting for reducing the levels of stress hormones in free ranging spider monkeys. [ABSTRACT FROM AUTHOR]

Published
2016
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27. Increased B and T Cell Responses in M. bovis Bacille Calmette-Guérin Vaccinated Pigs Co-Immunized with Plasmid DNA Encoding a Prototype Tuberculosis Antigen.

Author

Bruffaerts, Nicolas, Pedersen, Lasse E., Vandermeulen, Gaëlle, Préat, Véronique, Stockhofe-Zurwieden, Norbert, Huygen, Kris, and Romano, Marta

Subjects
B cells, T cells, BCG vaccines, PROTOTYPES, TUBERCULOSIS vaccines, CD8 antigen
Abstract

The only tuberculosis vaccine currently available, bacille Calmette-Guérin (BCG) is a poor inducer of CD8+ T cells, which are particularly important for the control of latent tuberculosis and protection against reactivation. As the induction of strong CD8+ T cell responses is a hallmark of DNA vaccines, a combination of BCG with plasmid DNA encoding a prototype TB antigen (Ag85A) was tested. As an alternative animal model, pigs were primed with BCG mixed with empty vector or codon-optimized pAg85A by the intradermal route and boosted with plasmid delivered by intramuscular electroporation. Control pigs received unformulated BCG. The BCG-pAg85A combination stimulated robust and sustained Ag85A specific antibody, lymphoproliferative, IL-6, IL-10 and IFN-γ responses. IgG1/IgG2 antibody isotype ratio reflected the Th1 helper type biased response. T lymphocyte responses against purified protein derivative of tuberculin (PPD) were induced in all (BCG) vaccinated animals, but responses were much stronger in BCG-pAg85A vaccinated pigs. Finally, Ag85A-specific IFN-γ producing CD8+ T cells were detected by intracellular cytokine staining and a synthetic peptide, spanning Ag85A131-150 and encompassing two regions with strong predicted SLA-1*0401/SLA-1*0801 binding affinity, was promiscuously recognized by 6/6 animals vaccinated with the BCG-pAg85A combination. Our study provides a proof of concept in a large mammalian species, for a new Th1 and CD8+ targeting tuberculosis vaccine, based on BCG-plasmid DNA co-administration. [ABSTRACT FROM AUTHOR]

Published
2015
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28. Parasites and steroid hormones: corticosteroid and sex steroid synthesis, their role in the parasite physiology and development.

Author

Romano, Marta C., Miranda-Brito, Carolina, Valdez, Ricardo A., and Jiménez, Pedro

Subjects
PARASITES, STEROID hormones, STEROID synthesis, TAENIASIS, ORGANS (Anatomy)
Abstract

In many cases parasites display highly complex life cycles that include the penetration and permanence of the larva or adults within host organs, but even in those that only have one host, reciprocal, intricate interactions occur. Evidence indicates that steroid hormones have an influence on the development and course of parasitic infections. The host gender's susceptibility to infection, and the related differences in the immune response are good examples of the host-parasite interplay. However, the capacity of these organisms to synthesize their own steroidogenic hormones still has more questions than answers. It is now well-known that many parasites synthesize ecdysteroids, but limited information is available on sex steroid and corticosteroid synthesis. This review intends to summarize some of the existing information in the field. In most, but not all parasitosis the host's hormonal environment determines the susceptibility, the course, and severity of parasite infections. In most cases the infection disturbs the host environment, and activates immune responses that end up affecting the endocrine system. Furthermore, sex steroids and corticosteroids may also directly modify the parasite reproduction and molting. Available information indicates that parasites synthesize some steroid hormones, such as ecdysteroids and sex steroids, and the presence and activity of related enzymes have been demonstrated. More recently, the synthesis of corticosteroid-like compounds has been shown in Taenia solium cysticerci and tapeworms, and in Taenia crassiceps WFU cysticerci. In-depth knowledge of the parasite's endocrine properties will contribute to understand their reproduction and reciprocal interactions with the host, and may also help designing tools to combat the infection in some clinical situations. [ABSTRACT FROM AUTHOR]

Published
2015
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29. Mice genetically inactivated in interleukin-17 A receptor are defective in long-term control of Mycobacterium tuberculosis infection.

Author

Freches, Danielle, Korf, Hannelie, Denis, Olivier, Havaux, Xavier, Huygen, Kris, and Romano, Marta

Subjects
MYCOBACTERIUM tuberculosis, INTERLEUKIN-17, LABORATORY mice, CYTOKINES, CELLULAR signal transduction, TUMOR necrosis factors, NEUTROPHILS, IMMUNITY, GENETICS
Abstract

Interleukin-17A ( IL-17A), a pro-inflammatory cytokine acting on neutrophil recruitment, is known to play an important role during Mycobacterium tuberculosis infection, but the role of IL-17 A receptor signalling in immune defence against this intracellular pathogen remains poorly documented. Here we have analysed this signalling using C57 BL/6 mice genetically inactivated in the IL-17 receptor A subunit ( IL-17 RA−/−). Although early after infection bacterial growth was controlled to the same extent as in wild-type mice, IL-17 RA−/− mice were defective in exerting long-term control of M. tuberculosis infection, as demonstrated by a progressively increasing pulmonary bacterial burden and shortened survival time. Compared with infected wild-type mice, IL-17 RA−/− mice showed impaired recruitment of neutrophils to the lungs at the early but not the late stage of infection. Pulmonary tumour necrosis factor-α, IL-6 and particularly IL-10 levels were decreased in the absence of IL-17 RA signalling, whereas IL-1β was increased. CD4+-mediated and γδ-mediated IL-17 A production was dramatically increased in IL-17 RA−/− mice (confirming part of their phenotype), whereas production of interferon-γ and expression of the bactericidal enzyme inducible nitric oxide synthase were not affected. Collectively, our data suggest that early but not late neutrophil recruitment is essential for IL-17 A-mediated long-term control of M. tuberculosis infection and that a functional interferon-γ response is not sufficient to control M. tuberculosis growth when the IL-17 RA pathway is deficient. As treatment of auto-immune diseases with anti- IL-17 A antibodies is actually being tested in clinical studies, our data suggest that caution should be taken with respect to possible reactivation of tuberculosis. [ABSTRACT FROM AUTHOR]

Published
2013
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30. Effects of adrenocorticotropic hormone challenge and age on hair cortisol concentrations in dairy cattle.

Author

González-de-la-Vara, Marcela del Rosario, Valdez, Ricardo Arturo, Lemus-Ramirez, Vicente, Vázquez-Chagoyán, Juan Carlos, Villa-Godoy, Alejandro, and Romano, Marta C.

Subjects
ADRENOCORTICOTROPIC hormone, HYDROCORTISONE, DAIRY cattle, HAIR, COWS, EFFECT of stress on animals
Abstract

The article presents a study on the effects of adrenocotropic hormone (ACTH) challenge and age on hair cortisol concentrations in dairy cattle. The researchers compared cortisol concentrations in the hair of cows and calves to test whether cortisol accumulates in bovine hair after ACTH challenges and to determine any link between cortisol levels and hair color in Holstein cows. Assessing cortisol concentration in hair is said to be a useful non-invasive method for assessing stress in cattle.

Published
2011

31. Experimental Tuberculosis in the Wistar Rat: A Model for Protective Immunity and Control of Infection.

Author

Singhal, Amit, Aliouat, El Moukhtar, Hervé, Maxime, Mathys, Vanessa, Kiass, Mehdi, Creusy, Colette, Delaire, Baptiste, Tsenova, Liana, Fleurisse, Laurence, Bertout, Julie, Camacho, Luis, Foo, Damian, Hui Chien Tay, Jie Yee Siew, Boukhouchi, Warda, Romano, Marta, Mathema, Barun, Dartois, Véronique, Kaplan, Gilla, and Bifani, Pablo

Subjects
TUBERCULOSIS in animals, TUBERCULOSIS prevention, LABORATORY rats, MICROBIAL virulence, ANIMAL models in research, RAT anatomy, LUNG diseases, GRANULOMA, IMMUNOSUPPRESSION
Abstract

Background: Despite the availability of many animal models for tuberculosis (TB) research, there still exists a need for better understanding of the quiescent stage of disease observed in many humans. Here, we explored the use of the Wistar rat model for the study of protective immunity and control of Mycobacterium tuberculosis (Mtb) infection. Methodology/Principal Findings: The kinetics of bacillary growth, evaluated by the colony stimulating assay (CFU) and the extent of lung pathology in Mtb infected Wistar rats were dependent on the virulence of the strains and the size of the infecting inoculums. Bacillary growth control was associated with induction of T helper type 1 (Th1) activation, the magnitude of which was also Mtb strain and dose dependent. Histopathology analysis of the infected lungs demonstrated the formation of well organized granulomas comprising epithelioid cells, multinucleated giant cells and foamy macrophages surrounded by large numbers of lymphocytes. The late stage subclinical form of disease was reactivated by immunosuppression leading to increased lung CFU. Conclusion: The Wistar rat is a valuable model for better understanding host-pathogen interactions that result in control of Mtb infection and potentially establishment of latent TB. These properties together with the ease of manipulation, relatively low cost and well established use of rats in toxicology and pharmacokinetic analyses make the rat a good animal model for TB drug discovery. [ABSTRACT FROM AUTHOR]

Published
2011
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32. INFLUENCIA DE LA TESTOSTERONA SOBRE LA INFECCIÓN CAUSADA POR TRYPANOSOMA CRUZI.

Author

Pérez, Ana Rosa, Pascutti, María Fernanda, Fontanella, Germán H., Martín, Ana P., Tartalini, Vanina, Nocito, Ana Lía, Berra, Héctor H., Pezzotto, Stella M., Romano, Marta C., and Revelli, Silvia S.

Abstract

Copyright of Revista Médica de Rosario is the property of Circulo Medico de Rosario and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2009

34. Impact of COVID-19 on the oncological outcomes of colorectal cancer surgery in northern Italy in 2019 and 2020: multicentre comparative cohort study.

Author

Rottoli, Matteo, Pellino, Gianluca, Spinelli, Antonino, Flacco, Maria E., Manzoli, Lamberto, Morino, Mario, Pucciarelli, Salvatore, Jovine, Elio, Hilal, Moh'd Abu, Rosati, Riccardo, Ferrero, Alessandro, Pietrabissa, Andrea, Guaglio, Marcello, Manzini, Nicolò de, Pilati, Pierluigi, Cassinotti, Elisa, Pignata, Giusto, Goletti, Orlando, Opocher, Enrico, and Danelli, Piergiorgio

Subjects
COLORECTAL cancer, ONCOLOGIC surgery, PROCTOLOGY, CANCER prognosis, COHORT analysis, ODDS ratio
Abstract

Background This study compared patients undergoing colorectal cancer surgery in 20 hospitals of northern Italy in 2019 versus 2020, in order to evaluate whether COVID-19-related delays of colorectal cancer screening resulted in more advanced cancers at diagnosis and worse clinical outcomes. Method This was a retrospective multicentre cohort analysis of patients undergoing colorectal cancer surgery in March to December 2019 versus March to December 2020. Independent predictors of disease stage (oncological stage, associated symptoms, clinical T4 stage, metastasis) and outcome (surgical complications, palliative surgery, 30-day death) were evaluated using logistic regression. Results The sample consisted of 1755 patients operated in 2019, and 1481 in 2020 (both mean age 69.6 years). The proportion of cancers with symptoms, clinical T4 stage, liver and lung metastases in 2019 and 2020 were respectively: 80.8 versus 84.5 per cent; 6.2 versus 8.7 per cent; 10.2 versus 10.3 per cent; and 3.0 versus 4.4 per cent. The proportions of surgical complications, palliative surgery and death in 2019 and 2020 were, respectively: 34.4 versus 31.9 per cent; 5.0 versus 7.5 per cent; and 1.7 versus 2.4 per cent. Cancers in 2020 (versus 2019) were more likely to be symptomatic (odds ratio 1.36 (95 per cent c.i. 1.09 to 1.69)), clinical T4 stage (odds ratio 1.38 (95 per cent c.i. 1.03 to 1.85)) and have multiple liver metastases (odds ratio 2.21 (95 per cent c.i. 1.24 to 3.94)), but were not more likely to be associated with surgical complications (odds ratio 0.79 (95 per cent c.i. 0.68 to 0.93)). Conclusion Colorectal cancer patients who had surgery between March and December 2020 had an increased risk of advanced disease in terms of associated symptoms, cancer location, clinical T4 stage and number of liver metastases. [ABSTRACT FROM AUTHOR]

Published
2022
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35. Cancer Treatment and Research During the COVID-19 Pandemic: Experience of the First 6 Months.

Author

de las Heras, Begoña, Saini, Kamal S., Boyle, Frances, Ades, Felipe, de Azambuja, Evandro, Bozovic-Spasojevic, Ivana, Romano, Marco, Capelan, Marta, Prasad, Rajeev, Pattu, Pugazhenthi, Massard, Christophe, Portera, Chia, Saini, Monika Lamba, Singh, Brajendra Prasad, Venkitaraman, Ramachandran, McNally, Richard, Leone, Manuela, Grande, Enrique, and Gupta, Sudeep

Subjects
COVID-19 pandemic, COVID-19, CANCER research, CANCER treatment, CANCER-related mortality, PANDEMICS, EARLY detection of cancer
Abstract

The coronavirus disease-2019 (COVID-19) pandemic has had a significant impact on patients with underlying malignancy. In this article, we summarize emerging data related to patients with cancer and COVID-19. Among patients with COVID-19, a higher proportion have an underlying diagnosis of cancer than seen in the general population. Also, patients with malignancy are likely to be more vulnerable than the general population to contracting COVID-19. Mortality is significantly higher in patients with both cancer and COVID-19 compared with the overall COVID-19-positive population. The early months of the pandemic saw a decrease in cancer screening and diagnosis, as well as postponement of standard treatments, which could lead to excess deaths from cancer in the future. [ABSTRACT FROM AUTHOR]

Published
2020
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36. Comparison of Imported Plasmodium ovale curtisi and P. ovale wallikeri Infections among Patients in Spain, 2005-2011.

Author

Rojo-Marcos, Gerardo, Rubio-Muñoz, José Miguel, Ramírez-Olivencia, Germán, García-Bujalance, Silvia, Elcuaz-Romano, Rosa, Díaz-Menéndez, Marta, Calderón, María, García-Bermejo, Isabel, Manuel Ruiz-Giardín, José, Merino-Fernández, Francisco Jesús, Torrús-Tendero, Diego, Delgado-Iribarren, Alberto, Ribell-Bachs, Mónica, Arévalo-Serrano, Juan, and Cuadros-González, Juan

Subjects
PLASMODIUM, NUCLEOTIDE sequence, INFECTION, HEMOLYSIS & hemolysins, ALBUMINS
Abstract

Sequencing data from Plasmodium ovale genotypes co-circulating in multiple countries support the hypothesis that P. ovale curtisi and P. ovale wallikeri are 2 separate species. We conducted a multicenter, retrospective, comparative study in Spain of 21 patients who had imported P. ovale curtisi infections and 14 who had imported P. ovale wallikeri infections confirmed by PCR and gene sequencing during June 2005-December 2011. The only significant finding was more severe thrombocytopenia among patients with P. ovale wallikeri infection than among those with P. ovale curtisi infection (p = 0.031). However, we also found nonsignificant trends showing that patients with P. ovale wallikeri infection had shorter time from arrival in Spain to onset of symptoms, lower level of albumin, higher median maximum core temperature, and more markers of hemolysis than did those with P. ovale curtisi infection. Larger, prospective studies are needed to confirm these findings. [ABSTRACT FROM AUTHOR]

Published
2014
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37. Development of a glycoconjugate vaccine to prevent meningitis in Africa caused by meningococcal serogroup X.

Author

Micoli, Francesca, Romano, Maria Rosaria, Tontini, Marta, Cappelletti, Emilia, Gavini, Massimiliano, Proietti, Daniela, Rondini, Simona, Swennen, Erwin, Santini, Laura, Filippini, Sara, Balocchi, Cristiana, Adamo, Roberto, Pluschke, Gerd, Norheim, Gunnstein, Pollard, Andrew, Saul, Allan, Rappuoli, Rino, MacLennan, Calman A., Berti, Francesco, and Costantino, Paolo

Subjects
NEISSERIA meningitidis, MENINGOCOCCAL vaccines, GLYCOCONJUGATES, OLIGOSACCHARIDES, LABORATORY mice, PREVENTION, THERAPEUTICS
Abstract

Neisseria meningitidis is a major cause of bacterial meningitis worldwide, especially in the African meningitis belt, and has a high associated mortality. The meningococcal serogroups A, W, and X have been responsible for epidemics and almost all cases of meningococcal meningitis in the meningitis belt over the past 12 y. Currently no vaccine is available against meningococcal X (MenX). Because the development of a new vaccine through to licensure takes many years, this leaves Africa vulnerable to new epidemics of MenX meningitis at a time when the epidemiology of meningococcal meningitis on the continent is changing rapidly, following the recent introduction of a glycoconjugate vaccine against serogroup A. Here, we report the development of candidate glycoconjugate vaccines against MenX and preclinical data from their use in animal studies. Following optimization of growth conditions of our seed MenX strain for polysaccharide (PS) production, a scalable purification process was developed yielding high amounts of pure MenX PS. Different glycoconjugates were synthesized by coupling MenX oligosaccharides of varying chain length to CRM197 as carrier protein. Analytical methods were developed for in-process control and determination of purity and consistency of the vaccines. All conjugates induced high anti-MenX PS lgG titers in mice. Antibodies were strongly bactericidal against African MenX isolates. These findings support the further development of glycoconjugate vaccines against MenX and their assessment in clinical trials to produce a vaccine against the one cause of epidemic meningococcal meningitis that currently cannot be prevented by available vaccines. [ABSTRACT FROM AUTHOR]

Published
2013
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39. A Propensity Score-Matched Analysis to Assess the Outcomes in Pre- and Post-Fast-Track Hip and Knee Elective Prosthesis Patients.

Author

Romano, Luigi U., Rigoni, Marta, Torri, Emanuele, Nella, Marilena, Morandi, Monica, Casetti, Piergiorgio, Nollo, Giandomenico, and Winkler, Tobias

Subjects
TOURNIQUETS, ARTIFICIAL knees, LENGTH of stay in hospitals, PERIOPERATIVE care, KNEE surgery, TOTAL hip replacement
Abstract

Fast-track surgery is a multimodal evidence-based approach to perioperative care aimed at reducing complications and recovery time. We compared a fast-track protocol to standard care in the setting of a small Italian general hospital. Propensity score estimation before and after the study was performed to compare pre-fast-track (pre-FT; January 2013–March 2014) and fast-track (FT; January 2016–December 2016) patients undergoing elective hip and knee replacement surgery with a three-year follow-up (up to January 2020). The primary endpoints were the mean hemoglobin drop, mean predischarge hemoglobin, transfusion and reinfusion rates, pain, ambulation day, hospital length of stay (LOS), and discharge to home/outpatient care or rehabilitation hospital center. The secondary endpoints were the adherence measures to the FT protocol, namely, tourniquet and surgical times, use of drains and catheters, type of anesthesia administered, and complications within three years. The risk difference (RD) and the adjusted odds ratio (aOR) were calculated for each outcome. After the propensity score estimation, we analyzed 59 patients in the pre-FT and 122 in the FT categories. The FT patients, with respect to the pre-FT patients, ameliorated their mean hemoglobin drop from 3.7 to 3.1 g/dl (p < 0.01) and improved their predischarge mean hemoglobin (10.5 g/dL versus 11.0 g/dL; p = 0.01). Furthermore, the aOR of being transfused was reduced by 81% (p < 0,01); the RD of being reinfused was reduced by 63% (p < 0.01); the aOR of having low pain on the first day was increased by more than six times (p < 0.01); the RD of ambulating the first day increased by 91% (p < 0.01); the aOR of admission to a rehabilitation hospital center was reduced by 98% (p < 0.01); the aOR of home discharge increased by 42 times (p < 0.01); the median LOS, tourniquet and surgical times, and use of catheters and drains significantly decreased. Patients with complications at 1 month were 43.1% and 38.2%, respectively, of pre-FT and FT patients (p = 0.63). Complications at 6, 12, 24, and 36 months were significantly lower for the FT patients. This study showed that the uptake of enhanced recovery practices was successful and resulted in the improvement of clinical and organizational outcomes. The fast-track concept and related programs may optimize perioperative care and streamline surgical and rehabilitation care paths. [ABSTRACT FROM AUTHOR]

Published
2021
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40. Optimised LAMP allows single copy detection of 35Sp and NOSt in transgenic maize using Bioluminescent Assay in Real Time (BART).

Author

Hardinge, Patrick, Kiddle, Guy, Tisi, Laurence, and Murray, James A. H.

Abstract

Loop-mediated amplification (LAMP) has been widely used to amplify and hence detect nucleic acid target sequences from various pathogens, viruses and genetic modifications. Two distinct types of primer are required for LAMP; hairpin-forming LAMP and displacement. High specificity arises from this use of multiple primers, but without optimal conditions for LAMP, sensitivity can be poor. We confirm here the importance of LAMP primer design, concentrations and ratios for efficient LAMP amplification. We further show that displacement primers are non-essential to the LAMP reaction at certain concentrations providing accelerating loop primers are present. We investigate various methods to quantify DNA extracts from GM maize certified reference materials to calculate the target copy numbers of template presented to the LAMP reaction, and show that LAMP can amplify transgenic promoter/terminator sequences in DNA extracted from various maize GM events using primers designed to target the 35S promoter (35Sp) or NOS terminator (NOSt) sequences, detection with both bioluminescence in real-time (BART) and fluorescent methods. With prior denaturation and HPLC grade LAMP primers single copy detection was achieved, showing that optimised LAMP conditions can be combined with BART for single copy targets, with simple and cost efficient light detection electronics over fluorescent alternatives. [ABSTRACT FROM AUTHOR]

Published
2018
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