Your search keyword '"Maria D. Flores"' showing total 7 results

1. Parasitemia Levels in Trypanosoma cruzi Infection in Spain, an Area Where the Disease Is Not Endemic: Trends by Different Molecular Approaches

Author

Maria D. Flores-Chavez, Alba Abras, Cristina Ballart, Ismael Ibáñez-Perez, Pilar Perez-Gordillo, Montserrat Gállego, Carmen Muñoz, Zaira Moure, Elena Sulleiro, Javier Nieto, Emilia García Diez, Lorena Simón, Israel Cruz, and Albert Picado

Subjects

Chagas disease, LAMP, Trypanosoma cruzi, acute reactivation, chronic infection, congenital infection, Microbiology, QR1-502

Abstract

ABSTRACT Trypanosoma cruzi infection has expanded globally through human migration. In Spain, the mother-to-child route is the mode of transmission contributing to autochthonous Chagas disease (CD); however, most people acquired the infection in their country of origin and were diagnosed in the chronic phase (imported chronic CD). In this context, we assessed the quantitative potential of the Loopamp Trypanosoma cruzi detection kit (Sat-TcLAMP) based on satellite DNA (Sat-DNA) to determine parasitemia levels compared to those detected by real-time quantitative PCRs (qPCRs) targeting Sat-DNA (Sat-qPCR) and kinetoplast DNA minicircles (kDNA-qPCR). This study included 173 specimens from 39 autochthonous congenital and 116 imported chronic CD cases diagnosed in Spain. kDNA-qPCR showed higher sensitivity than Sat-qPCR and Sat-TcLAMP. According to all quantitative approaches, parasitemia levels were significantly higher in congenital infection than in chronic CD (1 × 10−1 to 5 × 105 versus >1 × 10−1 to 6 × 103 parasite equivalents/mL, respectively [P

Published

2022

2. Fragment-Based Ab Initio Phasing of Peptidic Nanocrystals by MicroED

Author

Logan S. Richards, Maria D. Flores, Claudia Millán, Calina Glynn, Chih-Te Zee, Michael R. Sawaya, Marcus Gallagher-Jones, Rafael J. Borges, Isabel Usón, and Jose A. Rodriguez

Subjects

Drug Discovery, Pharmaceutical Science, Molecular Biology, Biochemistry

Published

2023

3. Cryo-EM Structure of a Human LECT2 Amyloid Fibril Reveals a Network of Polar Ladders at its Core

Author

Logan S. Richards, Maria D. Flores, Samantha Zink, Natalie A. Schibrowsky, Michael R. Sawaya, and Jose A. Rodriguez

Subjects

Article

Abstract

ALECT2 is a type of systemic amyloidosis caused by deposition of the leukocyte cell-derived chemotaxin-2 (LECT2) protein in the form of fibrils. In ALECT2, LECT2 fibril deposits can be found in the glomerulus, resulting in renal failure. Affected patients lack effective treatment options outside of renal transplant or dialysis. While the structure of LECT2 in its globular form has been determined by X-ray crystallography, structures of LECT2 amyloid fibrils remain unknown. Using single particle cryo-EM, we now find that human LECT2 forms robust twisting fibrils with canonical amyloid features. At their core, LECT2 fibrils contain two mating protofilaments, the ordered core of each protofilament spans residues 55-75 of the LECT2 sequence. The overall geometry of the LECT2 fibril displays features in line with other pathogenic amyloids. Its core is tightly packed and stabilized by a network of hydrophobic contacts and hydrogen-bonded uncharged polar residues, while its outer surface displays several charged residues. The robustness of LECT2 fibril cores is illustrated by their limited dissolution in 3M urea and their persistence after treatment with proteinase K. As such, the LECT2 fibril structure presents a potential new target for treatments against ALECT2.

Published

2023

4. Correction for Ferrero et al., 'Antibody-Based Inhibition of Pathogenic New World Hemorrhagic Fever Mammarenaviruses by Steric Occlusion of the Human Transferrin Receptor 1 Apical Domain'

Author

Sol Ferrero, Maria D. Flores, Connor Short, Cecilia A. Vazquez, Lars E. Clark, James Ziegenbein, Samantha Zink, Daniel Fuentes, Cristian Payes, María V. Batto, Michael Collazo, Cybele C. García, Jonathan Abraham, Sandra M. Cordo, Jose A. Rodriguez, and Gustavo Helguera

Subjects

Virology, Insect Science, Immunology, Microbiology

Published

2022

5. Fragment-based ab initio phasing of peptidic nanocrystals by MicroED

Author

Logan S. Richards, Rafael J. Borges, Jose A. Rodriguez, Calina Glynn, Marcus Gallagher-Jones, Chih-Te Zee, Claudia Millán, Maria D. Flores, Michael R. Sawaya, and Isabel Usón

Subjects

Synthetic protein, Crystallography, Materials science, Nanocrystal, Fragment (logic), Electron diffraction, Ab initio, Molecule, Phase problem, Phaser

Abstract

Microcrystal electron diffraction (MicroED) is transforming the visualization of molecules from nanocrystals, rendering their three-dimensional atomic structures from previously unamenable samples. Peptidic structures determined by MicroED include naturally occurring peptides, synthetic protein fragments and peptide-based natural products. However, as a diffraction method, MicroED is beholden to the phase problem, and its de novo determination of structures remains a challenge. ARCIMBOLDO, an automated, fragment-based approach to structure determination. It eliminates the need for atomic resolution, instead enforcing stereochemical constraints through libraries of small model fragments, and discerning congruent motifs in solution space to ensure validation. This approach expands the reach of MicroED to presently inaccessible peptidic structures including segments of human amyloids, and yeast and mammalian prions, and portends a more general phasing solution while limiting model bias for a wider set of chemical structures.

Published

2021

6. Fjord-Edge Graphene Nanoribbons with Site-Specific Nitrogen Substitution

Author

Julen Munarriz, Victoria M. Basile, Richard B. Kaner, Yolanda L. Li, Mit Muni, Maria D. Flores, Anastassia N. Alexandrova, Kendall N. Houk, Chih-Te Zee, Sarah H. Tolbert, Janice B. Lin, and Yves Rubin

Subjects

Models, Molecular, Nitrogen, Heteroatom, Biochemistry, Catalysis, law.invention, symbols.namesake, Colloid and Surface Chemistry, X-ray photoelectron spectroscopy, law, Models, Spectroscopy, Topology (chemistry), Nanotubes, Molecular Structure, Graphene, Chemistry, Nanotubes, Carbon, Molecular, General Chemistry, Carbon, Crystallography, Polymerization, Chemical Sciences, symbols, Graphite, Raman spectroscopy, Graphene nanoribbons

Abstract

The synthesis of graphene nanoribbons (GNRs) that contain site-specifically substituted backbone heteroatoms is one of the essential goals that must be achieved in order to control the electronic properties of these next generation organic materials. We have exploited our recently reported solid-state topochemical polymerization/cyclization-aromatization strategy to convert the simple 1,4-bis(3-pyridyl)butadiynes 3a,b into the fjord-edge nitrogen-doped graphene nanoribbon structures 1a,b (fjord-edge N2[8]GNRs). Structural assignments are confirmed by CP/MAS 13C NMR, Raman, and XPS spectroscopy. The fjord-edge N2[8]GNRs 1a,b are promising precursors for the novel backbone nitrogen-substituted N2[8]AGNRs 2a,b. Geometry and band calculations on N2[8]AGNR 2c indicate that this class of nanoribbons should have unusual bonding topology and metallicity.

Published

2020

7. HDP2: a ribosomal DNA (NTS-ETS) sequence as a target for species-specific molecular diagnosis of intestinal taeniasis in humans

Author

María D. Flores, Luis M. Gonzalez, Carolina Hurtado, Yamileth Monje Motta, Cristina Domínguez-Hidalgo, Francisco Jesús Merino, María J. Perteguer, and Teresa Gárate

Subjects

Taeniasis, Taenia solium, Taenia saginata, Diagnosis, cPCR, qPCR, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Taenia solium, T. asiatica and T. saginata tapeworms cause human taeniasis and are the origin of porcine and bovine cysticercosis. Furthermore, T. solium eggs can cause human cysticercosis, with neurocysticercosis being the most serious form of the disease. These helminth infections are neglected tropical diseases and are endemic in several countries in the Americas, Asia and Africa. As a result of globalization, migration in particular, the infections have been extending to non-endemic territories. Species-specific diagnosis of taeniasis is subject to drawbacks that could be resolved using molecular approaches. In the present study, conventional and real-time amplification protocols (cPCR and qPCR) based on the T. saginata HDP2 sequence were applied in the differential diagnosis of taeniasis (T. saginata, T. solium) in both fecal samples and proglottids expelled by patients. The HDP2 homolog in T. solium was cloned and characterized. Results Semi-nested cPCR and qPCR (Sn-HDP2 cPCR and Sn-HDP2 qPCR) amplified T. saginata and T. solium DNA, with an analytical sensitivity of 40 and 400 fg, respectively, and identically in both protocols. Eighteen taeniasis patients were diagnosed directly with T. saginata or T. solium, either from proglottids or fecal samples with/without eggs (detected using microscopy), based on the optimized Sn-HDP2 qPCR. After cloning, the T. solium HDP2 homolog sequence was confirmed to be a ribosomal sequence. The HDP2 fragment corresponded to a non-transcribed sequence/external transcribed repeat (NTS/ETS) of ribosomal DNA. Compared with the T. saginata HDP2 homolog, the T solium HDP2 sequence lacked the first 900 nt at the 5′ end and showed nucleotide substitutions and small deletions. Conclusions Sn-HDP2 cPCR and Sn-HDP2 qPCR were set up for the diagnosis of human taeniasis, using proglottids and fecal samples from affected patients. The new Sn-HDP2 qPCR protocol was the best option, as it directly differentiated T. saginata from T. solium. The diagnosis of an imported T. solium-taeniasis case and nine European T. saginata cases was relevant. Finally, the cloning and sequencing of the T. solium HDP2 fragment confirmed that HDP2 was part of a ribosomal unit.

Published

2018