Publications by authors named "Andrea Jurado"

Introduction: Bacteriophages have been shown to penetrate biofilms and replicate if they find suitable host cells. Therefore, these viruses appear to be a good option to tackle the biofilm problem and complement or even substitute more conventional antimicrobials. However, in order to successfully remove biofilms, in particular mature biofilms, phages may need to be administered along with other compounds.

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  • Flaviviruses like dengue, Zika, and yellow fever are transmitted by mosquitoes and cause diseases primarily in tropical regions, while Powassan virus (POWV) is tick-borne and found in temperate areas.
  • Research shows that people in Mexico and Brazil have neutralizing antibodies against POWV, suggesting possible exposure to the virus.
  • Monoclonal antibodies P002 and P003 target a shared epitope on POWV, hinting that POWV or a similar virus could infect humans in tropical locations.
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  • Lyme disease affects approximately 476,000 people annually in the U.S., presenting symptoms like rash and flu-like feelings, with varied outcomes that are not yet understood.
  • The study aimed to assess the presence of Powassan virus (POWV) antibodies in individuals with a history of Lyme disease, comparing those with low and high antibody levels.
  • Results showed discrepancies between antibody tests and no significant clinical symptom differences based on antibody levels, indicating challenges in diagnosing flavivirus exposure and highlighting the need for further research on potential co-infections.
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Background: Infections by the pathogen currently represent one of the most serious threats to human health worldwide, especially due to the production of enterotoxins and the ability to form biofilms. These structures and the acquisition of antibiotic resistance limit the action of antibiotics and disinfectants used to combat this microorganism in the industry and the clinic.

Methods: This work reports a comparative phenotypic and genotypic study of 18 strains from different origins: clinical samples, milk from mastitic cows and food industry surfaces, most of which were isolated in Northern Spain.

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The synthesis and characterization of ( PBP)Ni(OAc) (5) by insertion of carbon dioxide into the Ni-C bond of ( PBP)NiMe (1) is presented. An unexpected CO cleavage process involving the formation of new B-O and Ni-CO bonds leads to the generation of a butterfly-structured tetra-nickel cluster ( PBOP) Ni (μ-CO) (6). Mechanistic investigation of this reaction indicates a reductive scission of CO by O-atom transfer to the boron atom via a cooperative nickel-boron mechanism.

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Despite occurring at the microscopic scale, the armed race between phages and their bacterial hosts involves multiple mechanisms, some of which are just starting to be understood. On the one hand, bacteria have evolved strategies that can stop the viral infection at different stages (adsorption, DNA injection and replication, biosynthesis and assembly of the viral progeny and/or release of the newly formed virions); on the other, phages have gradually evolved counterattack strategies that allow them to continue infecting their prey. This co-evolutionary process has played a major role in the development of microbial populations in both natural and man-made environments.

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Despite the availability of a highly effective yellow fever virus (YFV) vaccine, outbreaks of yellow fever frequently occur in Africa and South America with significant mortality, highlighting the pressing need for antiviral drugs to manage future outbreaks. To support the discovery and development of antiviral drugs against YFV, we characterized a panel of rabbit polyclonal antibodies against the three YFV structural proteins and five non-structural proteins and demonstrated these antibody reagents in conjunction with viral RNA metabolic labeling, double-stranded RNA staining and membrane floatation assays as powerful tools for investigating YFV polyprotein processing, replication complex formation, viral RNA synthesis and high throughput discovery of antiviral drugs. Specifically, the proteolytic processing of the viral polyprotein can be analyzed by Western blot assays.

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Recent epidemics demonstrate the global threat of Zika virus (ZIKV), a flavivirus transmitted by mosquitoes. Although infection is usually asymptomatic or mild, newborns of infected mothers can display severe symptoms, including neurodevelopmental abnormalities and microcephaly. Given the large-scale spread, symptom severity, and lack of treatment or prophylaxis, a safe and effective ZIKV vaccine is urgently needed.

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Human infection by Zika virus (ZIKV) during pregnancy can lead to vertical transmission and fetal aberrations, including microcephaly. Prophylactic administration of antibodies can diminish or prevent ZIKV infection in animal models, but whether passive immunization can protect nonhuman primates and their fetuses during pregnancy has not been determined. Z004 and Z021 are neutralizing monoclonal antibodies to domain III of the envelope (EDIII) of ZIKV.

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Vaccination against measles, mumps, and rubella (MMR) and yellow fever (YF) with live attenuated viruses can rarely cause life-threatening disease. Severe illness by MMR vaccines can be caused by inborn errors of type I and/or III interferon (IFN) immunity (mutations in , , or ). Adverse reactions to the YF vaccine have remained unexplained.

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Cellular antiviral programs encode molecules capable of targeting multiple steps in the virus lifecycle. Zinc-finger antiviral protein (ZAP) is a central and general regulator of antiviral activity that targets pathogen mRNA stability and translation. ZAP is diffusely cytoplasmic, but upon infection ZAP is targeted to particular cytoplasmic structures, termed stress granules (SGs).

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