Your search keyword '"Sonia Mayra Pérez-Tapia"' showing total 112 results

1. Vaccination with Plasmids Encoding the Fusion Proteins D-S1, D-S1N and O-SN from SARS-CoV-2 Induces an Effective Humoral and Cellular Immune Response in Mice

Author

Noe Juvenal Mendoza-Ramírez, Julio García-Cordero, Gabriela Hernández-Galicia, Nicole Justine Moreno-Licona, Jesus Hernandez, Carlos Cabello-Gutierrez, Joaquín Alejandro Zúñiga-Ramos, Edgar Morales-Rios, Sonia Mayra Pérez-Tapia, Vianney Ortiz-Navarrete, Martha Espinosa-Cantellano, David Andrés Fernández-Benavides, and Leticia Cedillo-Barrón

Subjects

vaccine, nucleocapsid, plasmid DNA, fusion proteins, DNA immunization, Medicine

Abstract

Background: Next-generation vaccines against coronavirus disease 2019 (COVID-19) focus on inducing a long-lasting immune response against severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) and its emerging variants. To achieve this, antigens other than spike proteins have been proposed, and different platforms have been evaluated. Nucleic acid-based vaccines are fundamental for this process. Preclinical data have shown that the SARS-CoV-2 nucleocapsid protein induces a protective cellular immune response, and when combined with the spike protein, the resulting humoral and cellular immune responses are effective against some SARS-CoV-2 variants. Methods: We designed a DNA vaccine against the spike and nucleocapsid proteins of SARS-CoV-2 to generate fusion proteins based on the Delta and Omicron B.5 strains. The most immunogenic regions of the spike and nucleocapsid proteins of the Delta and Omicron B strains were selected using bioinformatics. The nucleotide sequences were cloned into pcDNA3.1, and named pcDNA3.1/D-S1, pcDNA3.1/D-S1N, and pcDNA3.1/O-SN. The immunogenicity of the generated fusion proteins was evaluated by analyzing the humoral and cellular responses elicited after the immunization of BALB/c mice. Results: DNA immunization induced antibody production, neutralization activity, and IFN-γ production. The inclusion of the nucleocapsid regions in the plasmid greatly enhanced the immune response. Moreover, cross-reactions with the variants of interest were confirmed. Conclusions: Plasmids-encoding fusion proteins combining the most immunogenic regions of the spike and nucleocapsid proteins present a promising strategy for designing new and effective vaccines against SARS-CoV-2.

Published

2025

2. Implementation of a roadmap for the comprehensive diagnosis, follow-up, and research of childhood leukemias in vulnerable regions of Mexico: results from the PRONAII Strategy

Author

Juan Carlos Núñez-Enríquez, Rubí Romo-Rodríguez, Pedro Gaspar-Mendoza, Gabriela Zamora-Herrera, Lizeth Torres-Pineda, Jiovanni Amador-Cardoso, Jebea A. López-Blanco, Laura Alfaro-Hernández, Lucero López-García, Arely Rosas-Cruz, Dulce Rosario Alberto-Aguilar, César Omar Trejo-Pichardo, Dalia Ramírez-Ramírez, Astin Cruz-Maza, Janet Flores-Lujano, Nuria Luna-Silva, Angélica Martínez-Martell, Karina Martínez-Jose, Anabel Ramírez-Ramírez, Juan Carlos Solis-Poblano, Patricia Zagoya-Martínez, Vanessa Terán-Cerqueda, Andrea Huerta-Moreno, Álvaro Montiel-Jarquín, Miguel Garrido-Hernández, Raquel Hernández-Ramos, Daniela Olvera-Caraza, Cynthia Shanat Cruz-Medina, Enoch Alvarez-Rodríguez, Lénica Anahí Chávez-Aguilar, Wilfrido Herrera-Olivares, Brianda García-Hidalgo, Lena Sarahí Cano-Cuapio, Claudia Guevara-Espejel, Gerardo Juárez-Avendaño, Juan Carlos Balandrán, Ma. del Rocío Baños-Lara, Mariana Cárdenas-González, Elena R. Álvarez-Buylla, Sonia Mayra Pérez-Tapia, Diana Casique-Aguirre, and Rosana Pelayo

Subjects

childhood leukemias, Mexico, measurable residual disease (MRD), diagnosis, vulnerable regions, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The main objective of the National Project for Research and Incidence of Childhood Leukemias is to reduce early mortality rates for these neoplasms in the vulnerable regions of Mexico. This project was conducted in the states of Oaxaca, Puebla, and Tlaxcala. A key strategy of the project is the implementation of an effective roadmap to ensure that leukemia patients are the target of maximum benefit of interdisciplinary collaboration between researchers, clinicians, surveyors, and laboratories. This strategy guarantees the comprehensive management of diagnosis and follow-up samples of pediatric patients with leukemia, centralizing, managing, and analyzing the information collected. Additionally, it allows for a precise diagnosis and monitoring of the disease through immunophenotype and measurable residual disease (MRD) studies, enhancing research and supporting informed clinical decisions for the first time in these regions through a population-based study. This initiative has significantly improved the diagnostic capacity of leukemia in girls, boys, and adolescents in the regions of Oaxaca, Puebla, and Tlaxcala, providing comprehensive, high-quality care with full coverage in the region. Likewise, it has strengthened collaboration between health institutions, researchers, and professionals in the sector, which contributes to reducing the impact of the disease on the community.

Published

2024

3. Epidemiology of childhood acute leukemias in marginalized populations of the central-south region of Mexico: results from a population-based registry

Author

Janet Flores-Lujano, Aldo Allende-López, David Aldebarán Duarte-Rodríguez, Erika Alarcón-Ruiz, Lizbeth López-Carrillo, Teresa Shamah-Levy, Mariano E. Cebrián, Ma. del Rocío Baños-Lara, Diana Casique-Aguirre, Jesús Elizarrarás-Rivas, Javier Antonio López-Aquino, Miguel Ángel Garrido-Hernández, Daniela Olvera-Caraza, Vanessa Terán-Cerqueda, Karina Beatriz Martínez-José, Pierre Mitchel Aristil-Chery, Enoch Alvarez-Rodríguez, Wilfrido Herrera-Olivares, Guillermo J. Ruíz-Arguelles, Lénica Anahí Chavez-Aguilar, Aquilino Márquez-Toledo, Lena Sarahi Cano-Cuapio, Nuria Citlalli Luna-Silva, Maria Angélica Martínez-Martell, Anabel Beatriz Ramirez-Ramirez, Laura Elizabeth Merino-Pasaye, César Alejandro Galván-Díaz, Aurora Medina-Sanson, Maria de Lourdes Gutiérrez-Rivera, Jorge Alfonso Martín-Trejo, Emmanuel Rodriguez-Cedeño, Vilma Carolina Bekker-Méndez, María de los Ángeles Romero-Tlalolini, Astin Cruz-Maza, Gerardo Juárez-Avendaño, Sonia Mayra Pérez-Tapia, Juan Carlos Rodríguez-Espinosa, Miriam Carmina Suárez-Aguirre, Fernando Herrera-Quezada, Anahí Hernández-Díaz, Lizbeth Alondra Galván-González, Minerva Mata-Rocha, Amanda Idaric Olivares-Sosa, Haydeé Rosas-Vargas, Silvia Jiménez-Morales, Mariana Cárdenas-González, María Elena Álvarez-Buylla Roces, Célida Duque-Molina, Rosana Pelayo, Juan Manuel Mejía-Aranguré, and Juan Carlos Núñez-Enriquez

Subjects

incidence, child, lymphoid leukemia, myeloid leukemia, registries, epidemiology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

IntroductionAcute leukemias (AL) are the main types of cancer in children worldwide. In Mexico, they represent one of the main causes of death in children under 20 years of age. Most of the studies on the incidence of AL in Mexico have been developed in the urban context of Greater Mexico City and no previous studies have been conducted in the central-south of the country through a population-based study. The aim of the present work was to identify the general and specific incidence rates of pediatric AL in three states of the south-central region of Mexico considered as some of the marginalized populations of Mexico (Puebla, Tlaxcala, and Oaxaca).MethodsA population-based study was conducted. Children aged less than 20 years, resident in these states, and newly diagnosed with AL in public/private hospitals during the period 2021-2022 were identified. Crude incidence rates (cIR), standardized incidence rates (ASIRw), and incidence rates by state subregions (ASIRsr) were calculated. Rates were calculated using the direct and indirect method and reported per million children under 20 years of age. In addition, specific rates were calculated by age group, sex, leukemia subtype, and immunophenotype.ResultsA total of 388 cases with AL were registered. In the three states, the ASIRw for AL was 51.5 cases per million (0-14 years); in Puebla, it was 53.2, Tlaxcala 54.7, and Oaxaca de 47.7. In the age group between 0-19 years, the ASIRw were 44.3, 46.4, 48.2, and 49.6, in Puebla, Tlaxcala, and Oaxaca, respectively. B-cell acute lymphoblastic leukemia was the most common subtype across the three states.ConclusionThe incidence of childhood AL in the central-south region of Mexico is within the range of rates reported in other populations of Latin American origin. Two incidence peaks were identified for lymphoblastic and myeloid leukemias. In addition, differences in the incidence of the disease were observed among state subregions which could be attributed to social factors linked to the ethnic origin of the inhabitants. Nonetheless, this hypothesis requires further investigation.

Published

2024

4. Subclassification of B-acute lymphoblastic leukemia according to age, immunophenotype and microenvironment, predicts MRD risk in Mexican children from vulnerable regions

Author

Rubí Romo-Rodríguez, Gabriela Zamora-Herrera, Jebea A. López-Blanco, Lucero López-García, Arely Rosas-Cruz, Laura Alfaro-Hernández, César Omar Trejo-Pichardo, Dulce Rosario Alberto-Aguilar, Diana Casique-Aguirre, Armando Vilchis-Ordoñez, Juan Carlos Solis-Poblano, Lilia Adela García-Stivalet, Vanessa Terán-Cerqueda, Nuria Citlalli Luna-Silva, Miguel Ángel Garrido-Hernández, Lena Sarahí Cano-Cuapio, Karen Ayala-Contreras, Fabiola Domínguez, María de los Ángeles del Campo-Martínez, Gerardo Juárez-Avendaño, Juan Carlos Balandrán, Sonia Mayra Pérez-Tapia, Carlos Fernández-Giménez, Pedro A. Zárate-Rodríguez, Enrique López-Aguilar, Aurora Treviño-García, Célida Duque-Molina, Laura C. Bonifaz, Juan Carlos Núñez-Enríquez, Mariana Cárdenas-González, Elena R. Álvarez-Buylla, Dalia Ramírez-Ramírez, and Rosana Pelayo

Subjects

tumor microenvironment, risk stratification, ProB-ALL, measurable residual disease (MRD), Mexican children, acute leukemia, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

IntroductionThe decisive key to disease-free survival in B-cell precursor acute lymphoblastic leukemia in children, is the combination of diagnostic timeliness and treatment efficacy, guided by accurate patient risk stratification. Implementation of standardized and high-precision diagnostic/prognostic systems is particularly important in the most marginalized geographic areas in Mexico, where high numbers of the pediatric population resides and the highest relapse and early death rates due to acute leukemias are recorded even in those cases diagnosed as standard risk.MethodsBy using a multidimensional and integrated analysis of the immunophenotype of leukemic cells, the immunological context and the tumor microenvironment, this study aim to capture the snapshot of acute leukemia at disease debut of a cohort of Mexican children from vulnerable regions in Puebla, Oaxaca and Tlaxcala and its potential use in risk stratification.Results and discussionOur findings highlight the existence of a distinct profile of ProB-ALL in children older than 10 years, which is associated with a six-fold increase in the risk of developing measurable residual disease (MRD). Along with the absence of CD34+ seminal cells for normal hematopoiesis, this ProB-ALL subtype exhibited several characteristics related to poor prognosis, including the high expression level of myeloid lineage markers such as MPO and CD33, as well as upregulation of CD19, CD34, CD24, CD20 and nuTdT. In contrast, it showed a trend towards decreased expression of CD9, CD81, CD123, CD13, CD15 and CD21. Of note, the mesenchymal stromal cell compartment constituting their leukemic niche in the bone marrow, displayed characteristics of potential suppressive microenvironment, such as the expression of Gal9 and IDO1, and the absence of the chemokine CXCL11. Accordingly, adaptive immunity components were poorly represented. Taken together, our results suggest, for the first time, that a biologically distinct subtype of ProB-ALL emerges in vulnerable adolescents, with a high risk of developing MRD. Rigorous research on potential enhancing factors, environmental or lifestyle, is crucial for its detection and prevention. The use of the reported profile for early risk stratification is suggested.

Published

2024

5. Use of Extracellular Monomeric Ubiquitin as a Therapeutic Option for Major Depressive Disorder

Author

José Luis Maldonado-García, Lissette Haydee García-Mena, Danelia Mendieta-Cabrera, Gilberto Pérez-Sánchez, Enrique Becerril-Villanueva, Samantha Alvarez-Herrera, Toni Homberg, Luis Vallejo-Castillo, Sonia Mayra Pérez-Tapia, Martha C. Moreno-Lafont, Daniel Ortuño-Sahagún, and Lenin Pavón

Subjects

major depressive disorder, immunomodulator, inflammation, extracellular monomeric ubiquitin, therapeutic options based in small proteins, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Major depressive disorder (MDD) is a mood disorder that has become a global health emergency according to the World Health Organization (WHO). It affects 280 million people worldwide and is a leading cause of disability and financial loss. Patients with MDD present immunoendocrine alterations like cortisol resistance and inflammation, which are associated with alterations in neurotransmitter metabolism. There are currently numerous therapeutic options for patients with MDD; however, some studies suggest a high rate of therapeutic failure. There are multiple hypotheses explaining the pathophysiological mechanisms of MDD, in which several systems are involved, including the neuroendocrine and immune systems. In recent years, inflammation has become an important target for the development of new therapeutic options. Extracellular monomeric ubiquitin (emUb) is a molecule that has been shown to have immunomodulatory properties through several mechanisms including cholinergic modulation and the generation of regulatory T cells. In this perspective article, we highlight the influence of the inflammatory response in MDD. In addition, we review and discuss the evidence for the use of emUb contained in Transferon as a concomitant treatment with selective serotonin reuptake inhibitors (SSRIs).

Published

2024

6. An international comparative analysis and roadmap to sustainable biosimilar markets

Author

Khalid A. Alnaqbi, Agnès Bellanger, Alex Brill, Gilberto Castañeda-Hernández, Ana Clopés Estela, Olga Delgado Sánchez, Pilar García-Alfonso, Pius Gyger, Daniel Heinrich, Germain Hezard, Adriana Kakehasi, Cheryl Koehn, Olivier Mariotte, Francesco Mennini, Sonia Mayra Pérez-Tapia, Michele Pistollato, Rowan Saada, Tadanori Sasaki, George Tambassis, Marc Thill, Gustavo Werutsky, Tim Wilsdon, and Steven Simoens

Subjects

biosimilar, sustainability, policy, market access, comparative analysis, Therapeutics. Pharmacology, RM1-950

Abstract

Background: Although biosimilar uptake has increased (at a variable pace) in many countries, there have been recent concerns about the long-term sustainability of biosimilar markets. The aim of this manuscript is to assess the sustainability of policies across the biosimilar life cycle in selected countries with a view to propose recommendations for supporting biosimilar sustainability.Methods: The study conducted a comparative analysis across 17 countries from North America, South America, Asia-Pacific, Europe and the Gulf Cooperation Council. Biosimilar policies were identified and their sustainability was assessed based on country-specific reviews of the scientific and grey literature, validation by industry experts and 23 international and local non-industry experts, and two advisory board meetings with these non-industry experts.Results: Given that European countries tend to have more experience with biosimilars and more developed policy frameworks, they generally have higher sustainability scores than the other selected countries. Existing approaches to biosimilar manufacturing and R&D, policies guaranteeing safe and high-quality biosimilars, exemption from the requirement to apply health technology assessment to biosimilars, and initiatives counteracting biosimilar misconceptions are considered sustainable. However, biosimilar contracting approaches, biosimilar education and understanding can be ameliorated in all selected countries. Also, similar policies are sometimes perceived to be sustainable in some markets, but not in others. More generally, the sustainability of the biosimilar landscape depends on the nature of the healthcare system and existing pharmaceutical market access policies, the experience with biosimilar use and policies. This suggests that a general biosimilar policy toolkit that ensures sustainability does not exist, but varies from country to country.Conclusion: This study proposes a set of elements that should underpin sustainable biosimilar policy development over time in a country. At first, biosimilar policies should guarantee the safety and quality of biosimilars, healthy levels of supply and a level of cost savings. As a country gains experience with biosimilars, policies need to optimise uptake and combat any misconceptions about biosimilars. Finally, a country should implement biosimilar policies that foster competition, expand treatment options and ensure a sustainable market environment.

Published

2023

7. Identification of SARS-CoV-2 Main Protease Inhibitors Using Chemical Similarity Analysis Combined with Machine Learning

Author

Karina Eurídice Juárez-Mercado, Milton Abraham Gómez-Hernández, Juana Salinas-Trujano, Luis Córdova-Bahena, Clara Espitia, Sonia Mayra Pérez-Tapia, José L. Medina-Franco, and Marco A. Velasco-Velázquez

Subjects

chemoinformatics, COVID-19, SARS-CoV-2, Mpro, 3CLpro, virtual screening, Medicine, Pharmacy and materia medica, RS1-441

Abstract

SARS-CoV-2 Main Protease (Mpro) is an enzyme that cleaves viral polyproteins translated from the viral genome, which is critical for viral replication. Mpro is a target for anti-SARS-CoV-2 drug development. Herein, we performed a large-scale virtual screening by comparing multiple structural descriptors of reference molecules with reported anti-coronavirus activity against a library with >17 million compounds. Further filtering, performed by applying two machine learning algorithms, identified eighteen computational hits as anti-SARS-CoV-2 compounds with high structural diversity and drug-like properties. The activities of twelve compounds on Mpro’s enzymatic activity were evaluated by fluorescence resonance energy transfer (FRET) assays. Compound 13 (ZINC13878776) significantly inhibited SARS-CoV-2 Mpro activity and was employed as a reference for an experimentally hit expansion. The structural analogues 13a (ZINC4248385), 13b (ZNC13523222), and 13c (ZINC4248365) were tested as Mpro inhibitors, reducing the enzymatic activity of recombinant Mpro with potency as follows: 13c > 13 > 13b > 13a. Then, their anti-SARS-CoV-2 activities were evaluated in plaque reduction assays using Vero CCL81 cells. Subtoxic concentrations of compounds 13a, 13c, and 13b displayed in vitro antiviral activity with IC50 in the mid micromolar range. Compounds 13a–c could become lead compounds for the development of new Mpro inhibitors with improved activity against anti-SARS-CoV-2.

Published

2024

8. Increased survival in puppies affected by Canine Parvovirus type II using an immunomodulator as a therapeutic aid

Author

Adriana I. Muñoz, Luis Vallejo-Castillo, Ana Fragozo, Said Vázquez-Leyva, Lenin Pavón, Gilberto Pérez-Sánchez, Rodolfo Soria-Castro, Gabriela Mellado-Sánchez, Laura Cobos-Marin, and Sonia Mayra Pérez-Tapia

Subjects

Medicine, Science

Abstract

Abstract Canine parvovirus type II (CPV-2) infection induces canine parvoviral enteritis (CPE), which in turn promotes sepsis and systemic inflammatory response syndrome (SIRS). Mortality in this disease is usually registered within 48–72 h post-hospitalization, the critical period of the illness. It has been recently described that the use of an immunomodulator, whose major component is monomeric ubiquitin (mUb) without the last two glycine residues (Ub∆GG), in pediatric human patients with sepsis augments survival. It is known that CXCR4 is the cell receptor of extracellular ubiquitin in humans. This work aimed to explore the effect of one immunomodulator (human Dialyzable Leukocyte Extract-hDLE) as a therapeutic auxiliary in puppies with sepsis and SIRS induced by CPE. We studied two groups of puppies with CPV-2 infection confirmed by polymerase chain reaction. The first group received conventional treatment (CT) and vehicle (V), while the second group received CT plus the immunomodulator (I). We assessed both groups' survival, clinical condition, number of erythrocytes, neutrophils, and lymphocytes during the hospitalization period. In addition, hematocrit, hemoglobin, plasma proteins and cortisol values, as well as norepinephrine/epinephrine and serotonin concentration were determined. Puppies treated with CT + I showed 81% survival, mild clinical signs, and a significant decrease in circulating neutrophils and lymphocytes in the critical period of the treatment. In contrast, the CT + V group presented a survival of 42%, severe clinical status, and no improvement of the parameters evaluated in the critical period of the disease. We determined in silico that human Ub∆GG can bind to dog CXCR4. In conclusion, the administration of a human immunomodulator (0.5 mg/day × 5 days) to puppies with CPE under six months of age reduces the severity of clinical signs, increases survival, and modulates inflammatory cell parameters. Further studies are necessary to take full advantage of these clinical findings, which might be mediated by the human Ub∆GG to canine CXCR4 interaction.

Published

2021

9. Altered neutrophil-to-lymphocyte ratio in sepsis secondary to canine parvoviral enteritis treated with and without an immunomodulator in puppies

Author

Adriana I. Muñoz, José Luis Maldonado-García, Ana Fragozo, Luis Vallejo-Castillo, Amellalli Lucas-Gonzalez, Ismael Trejo-Martínez, Lenin Pavón, Gilberto Pérez-Sánchez, Laura Cobos-Marin, and Sonia Mayra Pérez-Tapia

Subjects

canine parvoviral enteritis, neutrophils, lymphocytes, cortisol, epinephrine, norepinephrine, Veterinary medicine, SF600-1100

Abstract

Neutrophil-to-lymphocyte ratio (NLR) is a cheap and easy-to-obtain biomarker that mirrors the balance between innate and adaptive immunity. Cortisol and catecholamines have been identified as major drivers of NLR. High cortisol levels increase neutrophils while simultaneously decreasing lymphocyte counts. Likewise, endogenous catecholamines may cause leukocytosis and lymphopenia. Thus, NLR allows us to monitor patient severity in conditions such as sepsis. Twenty-six puppies with sepsis secondary to canine parvoviral enteritis were treated with and without an immunomodulator. Our group determined the NLR and the plasmatic cortisol levels by chemiluminescence, and norepinephrine (NE) and epinephrine (E) by HPLC during the first 72 h of clinical follow-up. Our results showed that at admission puppies presented an NLR value of 1.8, cortisol of 314.9 nmol/L, NE 3.7, and E 3.3 pmol/mL. Both treatments decreased admission NLR values after 24 h of treatment. However, only the puppies treated with the immunomodulator (I) remained without significant changes in NLR (0.7–1.4) compared to the CT group, and that showed a significant difference (P < 0.01) in their NLR value (0.4–4.6). In addition, we found significant differences in the slope values between the admission and final values of NLR (P < 0.005), cortisol (P < 0.02), and E (P < 0.05) between treatments. Then, our data suggest that the immunomodulator positively affects the number of lymphocytes and neutrophils involved in NLR as well as major drivers like cortisol and epinephrine, which is reflected in clinical parameters and survival.

Published

2022

10. Combination of Recombinant Proteins S1/N and RBD/N as Potential Vaccine Candidates

Author

Noe Juvenal Mendoza-Ramírez, Julio García-Cordero, Sandra Paola Martínez-Frías, Daniela Roa-Velázquez, Rosendo Luria-Pérez, José Bustos-Arriaga, Jesús Hernández-Lopez, Carlos Cabello-Gutiérrez, Joaquín Alejandro Zúñiga-Ramos, Edgar Morales-Ríos, Sonia Mayra Pérez-Tapia, Martha Espinosa-Cantellano, and Leticia Cedillo-Barrón

Subjects

SARS-CoV-2, vaccine, nucleocapsid protein, spike protein, RBD domain, Medicine

Abstract

Despite all successful efforts to develop a COVID-19 vaccine, the need to evaluate alternative antigens to produce next-generation vaccines is imperative to target emerging variants. Thus, the second generation of COVID-19 vaccines employ more than one antigen from severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) to induce an effective and lasting immune response. Here, we analyzed the combination of two SARS-CoV-2 viral antigens that could elicit a more durable immune response in both T- and B-cells. The nucleocapsid (N) protein, Spike protein S1 domain, and receptor binding domain (RBD) of the SARS-CoV-2 spike surface glycoproteins were expressed and purified in a mammalian expression system, taking into consideration the posttranscriptional modifications and structural characteristics. The immunogenicity of these combined proteins was evaluated in a murine model. Immunization combining S1 or RBD with the N protein induced higher levels of IgG antibodies, increased the percentage of neutralization, and elevated the production of cytokines TNF-α, IFN-γ, and IL-2 compared to the administration of a single antigen. Furthermore, sera from immunized mice recognized alpha and beta variants of SARS-CoV-2, which supports ongoing clinical results on partial protection in vaccinated populations, despite mutations. This study identifies potential antigens for second-generation COVID-19 vaccines.

Published

2023

11. Patient-Derived Bone Marrow Spheroids Reveal Leukemia-Initiating Cells Supported by Mesenchymal Hypoxic Niches in Pediatric B-ALL

Author

Juan Carlos Balandrán, José Dávila-Velderrain, Antonio Sandoval-Cabrera, Gabriela Zamora-Herrera, Vanessa Terán-Cerqueda, Lilia Adela García-Stivalet, José Alejandro Limón-Flores, Erick Armenta-Castro, Aurora Rodríguez-Martínez, Bertha Alicia Leon-Chavez, Verónica Vallejo-Ruiz, Duane C. Hassane, Sonia Mayra Pérez-Tapia, Vianney Ortiz-Navarrete, Monica L. Guzman, and Rosana Pelayo

Subjects

acute lymphoblastic leukemia, leukemia-initiating cell, bone marrow niche, mesenchymal stromal cells, tumor microenvironment, B-cell development, Immunologic diseases. Allergy, RC581-607

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) results from the expansion of malignant lymphoid precursors within the bone marrow (BM), where hematopoietic niches and microenvironmental signals provide leukemia-initiating cells (LICs) the conditions to survive, proliferate, initiate disease, and relapse. Normal and malignant lymphopoiesis are highly dependent on the BM microenvironment, particularly on CXCL12-abundant Reticular (CAR) cells, which provide a niche for maintenance of primitive cells. During B-ALL, leukemic cells hijack BM niches, creating a proinflammatory milieu incompetent to support normal hematopoiesis but favoring leukemic proliferation. Although the lack of a phenotypic stem cell hierarchy is apparent in B-ALL, LICs are a rare and quiescent population potentially responsible for chemoresistance and relapse. Here, we developed novel patient-derived leukemia spheroids (PDLS), an ex vivo avatar model, from mesenchymal stromal cells (MSCs) and primary B-ALL cells, to mimic specialized niche structures and cell-to-cell intercommunication promoting normal and malignant hematopoiesis in pediatric B-ALL. 3D MSC spheroids can recapitulate CAR niche-like hypoxic structures that produce high levels of CXCL10 and CXCL11. We found that PDLS were preferentially enriched with leukemia cells displaying functional properties of LICs, such as quiescence, low reactive oxygen species, drug resistance, high engraftment in immunodeficient mice, and long-term leukemogenesis. Moreover, the combination of PDLS and patient-derived xenografts confirmed a microenvironment-driven hierarchy in their leukemic potential. Importantly, transcriptional profiles of MSC derived from primary patient samples revealed two unique signatures (1), a CXCL12low inflammatory and leukemia expansion (ILE)-like niche, that likely supports leukemic burden, and (2) a CXCL11hi immune-suppressive and leukemia-initiating cell (SLIC)-like niche, where LICs are likely sustained. Interestingly, the CXCL11+ hypoxic zones were recapitulated within the PDLS that are capable of supporting LIC functions. Taken together, we have implemented a novel PDLS system that enriches and supports leukemia cells with stem cell features driven by CXCL11+ MSCs within hypoxic microenvironments capable of recapitulating key features, such as tumor reemergence after exposure to chemotherapy and tumor initiation. This system represents a unique opportunity for designing ex vivo personalized avatars for B-ALL patients to evaluate their own LIC pathobiology and drug sensitivity in the context of the tumor microenvironment.

Published

2021

12. Effector-Memory B-Lymphocytes and Follicular Helper T-Lymphocytes as Central Players in the Immune Response in Vaccinated and Nonvaccinated Populations against SARS-CoV-2

Author

Lorenzo Islas-Vazquez, Marisa Cruz-Aguilar, Henry Velazquez-Soto, Aida Jiménez-Corona, Sonia Mayra Pérez-Tapia, and Maria C. Jimenez-Martinez

Subjects

SARS-CoV-2, vaccine, COVID-19, B-lymphocytes, follicular helper T-lymphocytes (TFH), Medicine

Abstract

Vaccines have been recognized as having a central role in controlling the COVID-19 pandemic; however, most vaccine development research is focused on IgG-induced antibodies. Here, we analyzed the generation of IgGs related to SARS-CoV-2 and the changes in B- and T-lymphocyte proportions following vaccination against COVID-19. We included samples from 69 volunteers inoculated with the Pfizer-BioNTech (BNT162b2), Astra Zeneca (AZD1222 Covishield), or Sputnik V (Gam-COVID-Vac) vaccines. IgGs related to SARS-CoV-2 increased after the first vaccine dose compared with the nonvaccinated group (Pfizer, p = 0.0001; Astra Zeneca, p < 0.0001; Sputnik V, p = 0.0089). The results of the flow cytometry analysis of B- and T-lymphocytes showed a higher proportion of effector-memory B-lymphocytes in both first and second doses when compared with the nonvaccinated subjects. FcRL4+ cells were increased in second-dose-vaccinated COVID-19(−) and recovered COVID-19(+) participants when compared with the nonvaccinated participants. COVID-19(−) participants showed a lower proportion of follicular helper T-lymphocytes (TFH) in the second dose when compared with the first-vaccine-dose and nonvaccinated subjects. In conclusion, after the first vaccine dose, immunization against SARS-CoV-2 induces IgG production, and this could be mediated by TFH and effector-memory B-lymphocytes. Our data can be used in the design of vaccine schedules to evaluate immuno-bridging from a cellular point of view.

Published

2022

13. Kinetic Changes in B7 Costimulatory Molecules and IRF4 Expression in Human Dendritic Cells during LPS Exposure

Author

Henry Velazquez-Soto, Fernanda Real-San Miguel, Sonia Mayra Pérez-Tapia, and María C. Jiménez-Martínez

Subjects

LPS, costimulatory molecules, dendritic cells, cytokines, PDL1, PDL2, Microbiology, QR1-502

Abstract

A key aspect of the inflammatory phenomenon is the involvement of costimulatory molecules expressed by antigen-presenting cells (APCs) and their ability to secrete cytokines to set instructions for an adaptive immune response and to generate tolerance or inflammation. In a novel integrative approach, we aimed to evaluate the kinetic expression of the membrane and soluble B7 costimulatory molecules CD86, ICOS-L, PDL1, PDL2, the transcription factor Interferon Regulatory Factor 4 (IRF4), and the cytokines produced by monocyte-derived dendritic cells (Mo-DCs) after challenging them with different concentrations of stimulation with E. coli lipopolysaccharide (LPS) for different lengths of time. Our results showed that the stimuli concentration and time of exposure to an antigen are key factors in modulating the dynamic expression pattern of membrane and soluble B7 molecules and cytokines.

Published

2022

14. Glycosylated Nanoparticles for Cancer-Targeted Drug Delivery

Author

Sergio Andrés Torres-Pérez, Cindy Estefani Torres-Pérez, Martha Pedraza-Escalona, Sonia Mayra Pérez-Tapia, and Eva Ramón-Gallegos

Subjects

drug delivery, glycoconjugates, glycosylated nanoparticles, glycodendrimers, cancer therapy, glycopolymers, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Nanoparticles (NPs) are novel platforms that can carry both cancer-targeting molecules and drugs to avoid severe side effects due to nonspecific drug delivery in standard chemotherapy treatments. Cancer cells are characterized by abnormal membranes, metabolic changes, the presence of lectin receptors, glucose transporters (GLUT) overexpression, and glycosylation of immune receptors of programmed death on cell surfaces. These characteristics have led to the development of several strategies for cancer therapy, including a large number of carbohydrate-modified NPs, which have become desirable for use in cell-selective drug delivery systems because they increase nanoparticle-cell interactions and uptake of carried drugs. Currently, the potential of NP glycosylation to enhance the safety and efficacy of carried therapeutic antitumor agents has been widely acknowledged, and much information is accumulating in this field. This review seeks to highlight recent advances in NP stabilization, toxicity reduction, and pharmacokinetic improvement and the promising potential of NP glycosylation from the perspective of molecular mechanisms described for drug delivery systems for cancer therapy. From preclinical proof-of-concept to demonstration of therapeutic value in the clinic, the challenges and opportunities presented by glycosylated NPs, with a focus on their applicability in the development of nanodrugs, are discussed in this review.

Published

2020

15. Sequencing Analysis and Identification of the Primary Peptide Component of the Dialyzable Leukocyte Extract 'Transferon Oral': The Starting Point to Understand Its Mechanism of Action

Author

Luis Vallejo-Castillo, Liliana Favari, Said Vázquez-Leyva, Gabriela Mellado-Sánchez, Zaira Macías-Palacios, Leonardo E. López-Juárez, Luis Valencia-Flores, Emilio Medina-Rivero, Rommel Chacón-Salinas, Lenin Pavón, and Sonia Mayra Pérez-Tapia

Subjects

Transferon, human dialyzable leukocyte extracts, MS sequencing, immunomodulatory drugs, oral peptides, monomeric ubiquitin, Therapeutics. Pharmacology, RM1-950

Abstract

“Transferon Oral” is a peptide-derived product with immunomodulatory properties obtained from the lysis and dialysis of human buffy coat. Its active pharmaceutical ingredient, generically known as Dialyzable Leucocyte Extract, is a mixture of peptide populations with reproducible proportions among batches. “Transferon Oral” modulates IFN-γ, TNF-α, and IL-6 and increases the survival rate in a herpes infection murine model when oropharyngeally (ORO) administered, which correlate with clinical observations where “Transferon Oral” is used as a therapeutic auxiliary in inflammatory diseases. Notwithstanding, how a peptide-derived product elicits systemic modulation of cytokines when ORO administered remains unclear. To shed light on the pharmacology of “Transferon Oral” its peptide components must be known. Ten “Transferon Oral” batches were sequenced by mass spectrometry and the intact peptides were identified. The most abundant peptides were the monomeric human Ubiquitin (Ub), a globular low-molecular mass protein, and an Ub variant which lacks the two-terminal Gly (Ub-GG). Recombinant Ub prevented murine death when ORO administered in a herpes infection murine model. Besides, the percentage of survival increased in groups treated with Transferon Oral+Ub and decreased in groups treated with Ub-depleted “Transferon Oral” respect to the group treated with “Transferon Oral” only. Our findings indicate that the biological properties of “Transferon Oral” are partially associated to the Ub content. They suggest that Ub may activate its extracellular receptor (CXCR-4) in the stomach eliciting systemic immunomodulatory effects via vagus nerve. This is the first report that identifies an active component of “Transferon Oral” with the potential for the development of oral peptide immunomodulators.

Published

2020

16. IκBNS and IL-6 expression is differentially established in the uterus of pregnant healthy and infected mice

Author

Fernando Gómez-Chávez, Óscar Humberto López-Portales, Damariz Adriana Baeza-Martínez, Juan Carlos Cancino-Díaz, José Martín Murrieta-Coxca, Mario Eugenio Cancino-Díaz, Sonia Mayra Pérez-Tapia, and Sandra Rodríguez-Martínez

Subjects

Biological sciences, Immunology, Health sciences, Women's health, Reproductive system, IL-6, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

During pregnancy, NF-κB plays an important role for embryo implantation and the onset of labor. Regulated IL-6 production, under transcriptional control of NF-κB, is essential for a successful pregnancy outcome and the atypical regulator IκBNS is involved in this process. Previously, we showed that IκBNS negatively regulates IL-6 in uterine tissues during mouse estrous cycle. In this work, we analyzed if IκBNS and IL-6 expression in pregnant mice under physiological or L. monocytogenes-infected conditions would remain as observed in estrous cycle. In the healthy pregnancy IL-6 was highly expressed during implantation/placentation and labor stages but decreased during fetal development and post-partum stages. In contrast, in mice infected before pregnancy, IL-6 expression was not increased in the implantation stage, and its regulator IκBNS increased more in the infected condition rather than in the healthy pregnancy. IκBNS expression was reduced in post-implantation infection, allowing for IL-6 overexpression. The IκBNS-unrelated cytokine IL-36γ, used as inflammatory cytokine marker, was severely increased in the infected uterine tissues. When we analyzed the effect of infection over the fetuses, we found that pre-implantation infection caused the resorption (rejection) of some products, while the post-implantation infection restricted the intrauterine growth of fetuses. The results suggest that in the uterine tissue of pregnant mice the regulatory effect of IκBNS over IL-6 is more evident in an infection status rather than in a healthy condition.

Published

2020

17. Taking advantage of a high-throughput flow cytometer for the implementation of an ADCC assay for regulatory compliance

Author

Rosa Camacho-Sandoval, Alexis Jiménez-Uribe, Alejandra V. Tenorio-Calvo, Carlos A. López-Morales, Leslie Muñoz-García, Alejandra Montes-Luna, Héctor Leonardo García-Xolalpa, Marco Velasco-Velázquez, Lenin Pavón, Sonia Mayra Pérez-Tapia, and Emilio Medina-Rivero

Subjects

ADCC, High-throughput flow cytometry, Validation bioassay, Biotechnology, TP248.13-248.65

Abstract

Technological advances allowed the development of high-throughput instruments such as IntelliCyt iQue Screener PLUS®. Here, we took advantage of this technology to transfer a previously validated cytotoxicity assay. The evaluated parameters were cell permeability, caspase activation and phosphatidyl serine exposure. The assay was accurate (r2 = 0.90), precise (%CV ≤ 18.90) and specific. These results showed that this technology is suitable to be used in control quality environments. In addition, the automation provided a faster acquisition and analysis of data with precise and accurate results. This application could be implemented to evaluate another in vitro mechanism of action of different biotherapeutics.

Published

2020

18. Detection of CD39 and a Highly Glycosylated Isoform of Soluble CD73 in the Plasma of Patients with Cervical Cancer: Correlation with Disease Progression

Author

Ricardo Muñóz-Godínez, María de Lourdes Mora-García, Benny Weiss-Steider, Juan José Montesinos-Montesinos, Adriana del Carmen Aguilar-Lemarroy, Rosario García-Rocha, Jorge Hernández-Montes, Christian Azucena Don-López, Luis Roberto Ávila-Ibarra, Daniela Berenice Torres-Pineda, Gabriela Molina-Castillo, Rommel Chacón-Salinas, Luis Vallejo-Castillo, Sonia Mayra Pérez-Tapia, and Alberto Monroy-García

Subjects

Pathology, RB1-214

Abstract

Persistent infection with high-risk human papillomavirus (HR-HPV) is the main factor in the development of cervical cancer (CC). The presence of immunosuppressive factors plays an important role in the development of this type of cancer. To determine whether CD39 and CD73, which participate in the production of immunosuppressive adenosine (Ado), are involved in the progression of CC, we compared the concentrations and hydrolytic activity of these ectonucleotidases in platelet-free plasma (PFP) samples between patients with low-grade squamous intraepithelial lesions (LSILs) (n=18), high-grade squamous intraepithelial lesions (HSILs) (n=12), and CC (n=19) and normal donors (NDs) (n=15). The concentrations of CD39 and CD73 in PFP increased with disease progression (r=0.5929, p

Published

2020

19. Non‐biofilm‐forming commensal Staphylococcus epidermidis isolates produce biofilm in the presence of trypsin

Author

Sergio Martínez‐García, Silvestre Ortega‐Peña, María De Jesús De Haro‐Cruz, Ma. Guadalupe Aguilera‐Arreola, María Dolores Alcántar‐Curiel, Gabriel Betanzos‐Cabrera, Janet Jan‐Roblero, Sonia Mayra Pérez‐Tapia, Sandra Rodríguez‐Martínez, Mario E. Cancino‐Diaz, and Juan C. Cancino‐Diaz

Subjects

non‐biofilm‐forming, protease‐independent biofilm, Staphylococcus epidermidis, total biofilm, trypsin, Microbiology, QR1-502

Abstract

Abstract Epidemiological studies comparing clinical and commensal Staphylococcus epidermidis isolates suggest that biofilm formation is a discriminant biomarker. A study showed that four non‐biofilm‐forming clinical S. epidermidis isolates could form an induced biofilm by trypsin treatment, suggesting that S. epidermidis can form biofilms in a protease‐independent way and in a trypsin‐induced way. In this study, the trypsin capacity to induce biofilm formation was evaluated in non‐biofilm‐forming S. epidermidis isolates (n = 133) in order to support this mechanism and to establish the importance of total biofilms (meaning the sum of protease‐independent biofilm and trypsin‐induced biofilm). Staphylococcus epidermidis isolates from ocular infections (OI; n = 24), prosthetic joint infections (PJI; n = 64), and healthy skin (HS‐1; n = 100) were screened for protease‐independent biofilm formation according to Christensen's method. The result was that there are significant differences (p

Published

2019

20. Validation of a cell-based colorimetric reporter gene assay for the evaluation of Type I Interferons

Author

Ignacio Mejía-Calvo, Leslie Muñoz-García, Alexis Jiménez-Uribe, Rosa Camacho-Sandoval, Edith González-González, Gabriela Mellado-Sánchez, Alejandra V. Tenorio-Calvo, Carlos A. López-Morales, Marco A. Velasco-Velázquez, Lenin Pavón, Sonia Mayra Pérez-Tapia, and Emilio Medina-Rivero

Subjects

Biotechnology, TP248.13-248.65

Abstract

The biotherapeutic type I interferons (IFN-I) are indicated to treat several diseases. These products are regulated to guarantee safety and efficacy through critical quality attributes. For this purpose, the development of robust assays is required, followed by its validation to demonstrate their suitability for its intended purpose. Despite there are some commercial kits to evaluate IFN-I signaling, these are focused on measuring in vitro biological response instead of their validation, which is a pharmaceutical industry requirement. The aim of this work was to validate the HEK-Blue IFN-α/β system evaluating the biological activity of IFN-α/β under good laboratory practices, according to international standards. Our results demonstrated that HEK-Blue IFN-α/β system comply with accuracy (r2>0.95) precision (CV

Published

2019

21. Behavioral and Neurochemical Shifts at the Hippocampus and Frontal Cortex Are Associated to Peripheral Inflammation in Balb/c Mice Infected with Brucella abortus 2308

Author

José Luis Maldonado-García, Gilberto Pérez-Sánchez, Enrique Becerril Villanueva, Samantha Alvarez-Herrera, Lenin Pavón, Gabriel Gutiérrez-Ospina, Rubén López-Santiago, Jesús Octavio Maldonado-Tapia, Sonia Mayra Pérez-Tapia, and Martha C. Moreno-Lafont

Subjects

brucellosis, neurotransmitters, behavioral alterations, inflammation, brain regions, Biology (General), QH301-705.5

Abstract

Brucellosis is a zoonosis affecting 50,000,000 people annually. Most patients progress to a chronic phase of the disease in which neuropsychiatric symptoms upsurge. The biological processes underlying the progression of these symptoms are yet unclear. Peripheral inflammation mounted against Brucella may condition neurochemical shifts and hence unchained neuropsychiatric disorders. Our work aimed at establishing whether neurological, behavioral, and neurochemical disarrays are circumstantially linked to peripheral inflammation uprise secondary to Brucella abortus 2308 infections. We then evaluated, in control and Brucella-infected mice, skeletal muscle strength, movement coordination, and balance and motivation, as well as dopamine, epinephrine, norepinephrine, and serotonin availability in the cerebellum, frontal cortex, and hippocampus. Serum levels of proinflammatory cytokines and corticosterone in vehicle-injected and -infected mice were also estimated. All estimates were gathered at the infection acute and chronic phases. Our results showed that infected mice displayed motor disabilities, muscular weakness, and reduced motivation correlated with neurochemical and peripheral immunological disturbances that tended to decrease after 21 days of infection. The present observations support that disturbed peripheral inflammation and the related neurochemical disruption might lead to mood disorders in infected mice. Future experiments must be aimed at establishing causal links and to explore whether similar concepts might explain neurological and mood disorders in humans affected by brucellosis.

Published

2021

22. Transferon™, a peptide mixture with immunomodulatory properties is not immunogenic when administered with various adjuvants

Author

Sandra Avila, Leslie Muñoz-García, Said Vázquez-Leyva, Nohemí Salinas-Jazmín, Emilio Medina-Rivero, Lenin Pavón, Gabriela Mellado-Sánchez, Rommel Chacón-Salinas, Sergio Estrada-Parra, Luis Vallejo-Castillo, and Sonia Mayra Pérez-Tapia

Subjects

ADA, hDLE, immunogenicity, adjuvants, Transferon™, Immunologic diseases. Allergy, RC581-607, Toxicology. Poisons, RA1190-1270

Abstract

Transferon, a human dialyzable leukocyte extract (hDLE), is a biotherapeutic that comprises a complex mixture of low-molecular-weight peptides (

Published

2017

23. Development of Functional Antibodies Directed to Human Dialyzable Leukocyte Extract (Transferon®)

Author

Gabriela Mellado-Sánchez, Juan José Lázaro-Rodríguez, Sandra Avila, Luis Vallejo-Castillo, Said Vázquez-Leyva, Gregorio Carballo-Uicab, Marco Velasco-Velázquez, Emilio Medina-Rivero, Lenin Pavón, Rommel Chacón-Salinas, and Sonia Mayra Pérez-Tapia

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

Transferon® is an immunomodulator made of a complex mixture of peptides from human dialyzable leucocyte extracts (hDLEs). Development of surrogate antibodies directed to hDLE is an indispensable tool for studies during process control and preclinical trials. These antibodies are fundamental for different analytical approaches, such as identity test and drug quantitation, as well as to characterize its pharmacokinetic and mechanisms of action. A previous murine study showed the inability of the peptides of Transferon® to induce antibody production by themselves; therefore, in this work, two approaches were tested to increase its immunogenicity: chemical conjugation of the peptides of Transferon® to carrier proteins and the use of a rabbit model. Bioconjugates were generated with Keyhole Limpet Hemocyanin (KLH) or Bovine Serum Albumin (BSA) through maleimide-activated carrier proteins. BALB/c mice and New Zealand rabbits were immunized with Transferon® conjugated to KLH or nonconjugated Transferon®. Animals that were immunized with conjugated Transferon® showed significant production of antibodies as evinced by the recognition of Transferon®-BSA conjugate in ELISA assays. Moreover, rabbits showed higher antibody titers when compared with mice. Neither mouse nor rabbits developed antibodies when immunized with nonconjugated Transferon®. Interestingly, rabbit antibodies were able to partially block IL-2 production in Jurkat cells after costimulation with Transferon®. In conclusion, it is feasible to elicit specific and functional antibodies anti-hDLE with different potential uses during the life cycle of the product.

Published

2019

24. HPV-16 Infection Is Associated with a High Content of CD39 and CD73 Ectonucleotidases in Cervical Samples from Patients with CIN-1

Author

María de Lourdes Mora-García, Sofía López-Cisneros, Vianey Gutiérrez-Serrano, Rosario García-Rocha, Benny Weiss-Steider, Jorge Hernández-Montes, Héctor I. Sánchez-Peña, Luis Roberto Ávila-Ibarra, Christian Azucena Don-López, Ricardo Muñóz-Godínez, Daniela Berenice Torres Pineda, Rommel Chacón-Salinas, Luis Vallejo-Castillo, Sonia Mayra Pérez-Tapia, and Alberto Monroy-García

Subjects

Pathology, RB1-214

Abstract

The development of cervical cancer (CeCa) is associated with high-risk human papilloma virus (HR-HPV) infections, mainly HPV-16, which is present in more than 50% of cases. The presence of immunosuppressive factors in the early stages of the disease is also strongly linked to CeCa progression. In this context, it is unknown whether ectonucleotidases CD39 and CD73, which are involved in the production of adenosine (Ado) that suppresses the specific antitumor immune response, are present in precursor lesions of CeCa. In this pilot study, we analyzed the presence of CD39 and CD73 and their capacity to generate Ado in 25 cervical samples from patients with grade 1 cervical intraepithelial neoplasms (CIN-1) and 25 samples from normal donors (NDs) free of HPV infection. Cells obtained from cervical samples of CIN-1 patients positive for HPV-16 showed higher CD39 and CD73 contents compared to samples obtained from CIN-1 patients negative for HPV-16 and NDs. Interestingly, solubilized cervical mucus from these patients also showed higher contents of soluble CD39 and CD73, which were associated with a greater capacity to produce Ado from the hydrolysis of adenosine triphosphate (ATP) and adenosine monophosphate (AMP). In addition, serum samples of these patients showed higher levels of TGF-β than those of CIN-1 patients negative for HPV-16 and ND. These results suggest that persistent infection with HR-HPV, mostly HPV-16, in CIN-1 patients may promote the expression of CD39 and CD73 through the production of TGF-β in precursor lesions to generate an immunosuppressive microenvironment and allow its progression to CeCa.

Published

2019

25. Regulatory Pathway for Licensing Biotherapeutics in Mexico

Author

Carlos A. López-Morales, Alejandra Tenorio-Calvo, Rodolfo Cruz-Rodríguez, Julio Sánchez y Tepoz, Lahouari Belgharbi, Sonia Mayra Pérez-Tapia, and Emilio Medina-Rivero

Subjects

biotherapeutic products, harmonization, Common Technical Document, regulation, registration, licensing, Medicine (General), R5-920

Abstract

Biotherapeutic products which are derived from living organisms using recombinant DNA technology significantly contribute to the progress in the treatment of life-threatening and chronic diseases. The worldwide sale of biological drugs in 2016 was near US $263,700 million. In Latin America, where monoclonal antibodies market was worth US $7000 million, being Mexico the second largest market. Approval is one of the key aspects which influences the market of medicinal products, thus it is responsibility of the regulatory authority to establish a regulatory framework that ensure safety and efficacy of the products, and it is responsibility of the applicants to provide a high quality dossier in accordance with the registration requirements of the country. The applicants submitting registration requests in Mexico need to be aware of the requirements. Similar to many other countries, Mexico has adopted the Common Technical Document (CTD) structure for organizing dossier of the medicinal product for submission into main modules (i.e., quality, non-clinical, and clinical). This facilitates the submission process of medicinal products following a logical sequence aligned to the International Council on Harmonisation (ICH) guidelines. Moreover, this structure improves the transparency and clarity of the dossier in process of evaluation of medicinal products. In Mexico, the Ministry of Health has published a regulation, NOM-257-SSA1-2014, which established the general requirements to be followed by applicants to complete the registration of biotherapeutics. This regulation stipulates that the evaluation process is supported by a regulatory framework involving Good Manufacturing Practices, labeling, stability, clinical trials, biocomparability studies, pharmacovigilance, and a technical evaluation performed by a multidisciplinary team of experts in biotherapeutics development. Additionally, the Mexican regulatory agency, COFEPRIS, has published specific guidelines to facilitate the application process. Despite the availability of this information, the scope is limited to regulatory and administrative purposes, rather than technical-scientific supporting knowledge. The aim of this article is to provide concise information to improve and promote communication between industry and regulatory agencies. Herein, we describe the current process of COFEPRIS in regulating biotherapeutics in Mexico. This process explains the basis for the organization and structure of the technical-scientific information of biotherapeutics required for registration application.

Published

2018

26. Validation of a Cell Proliferation Assay to Assess the Potency of a Dialyzable Leukocyte Extract Intended for Batch Release

Author

Gregorio Carballo-Uicab, José E. Linares-Trejo, Gabriela Mellado-Sánchez, Carlos A. López-Morales, Marco Velasco-Velázquez, Lenin Pavón, Sergio Estrada-Parra, Sonia Mayra Pérez-Tapia, and Emilio Medina-Rivero

Subjects

dialyzable leukocyte extract, Transferon®, complex mixture of peptides, quality specifications, biological potency, development and validation, Organic chemistry, QD241-441

Abstract

Transferon® is a blood product with immunomodulatory properties constituted by a complex mixture of peptides obtained from a human dialyzable leukocyte extract (DLE). Due to its complex nature, it is necessary to demonstrate batch consistency in its biological activity. Potency is the quantitative measure of biological activity and is also a quality attribute of drugs. Here we developed and validated a proliferation assay using Jurkat cells exposed to azathioprine, which is intended to determine the potency of Transferon® according to international guidelines for pharmaceuticals. The assay showed a linear response (2.5 to 40 µg/mL), coefficients of variation from 0.7 to 13.6% demonstrated that the method is precise, while r2 = 0.97 between the nominal and measured values obtained from dilutional linearity showed that the method is accurate. We also demonstrated that the cell proliferation response was specific for Transferon® and was not induced by its vehicle nor by other peptide complex mixtures (glatiramer acetate or hydrolyzed collagen). The bioassay validated here was used to assess the relative potency of eight released batches of Transferon® with respect to a reference standard, showing consistent results. The collective information from the validation and the assessment of several batches indicate that the bioassay is suitable for the release of Transferon®.

Published

2019

27. Phage Display Libraries for Antibody Therapeutic Discovery and Development

Author

Juan C. Almagro, Martha Pedraza-Escalona, Hugo Iván Arrieta, and Sonia Mayra Pérez-Tapia

Subjects

naive repertoires, synthetic repertoires, antibody library design, developability, hit rate, affinity, Immunologic diseases. Allergy, RC581-607

Abstract

Phage display technology has played a key role in the remarkable progress of discovering and optimizing antibodies for diverse applications, particularly antibody-based drugs. This technology was initially developed by George Smith in the mid-1980s and applied by John McCafferty and Gregory Winter to antibody engineering at the beginning of 1990s. Here, we compare nine phage display antibody libraries published in the last decade, which represent the state of the art in the discovery and development of therapeutic antibodies using phage display. We first discuss the quality of the libraries and the diverse types of antibody repertoires used as substrates to build the libraries, i.e., naïve, synthetic, and semisynthetic. Second, we review the performance of the libraries in terms of the number of positive clones per panning, hit rate, affinity, and developability of the selected antibodies. Finally, we highlight current opportunities and challenges pertaining to phage display platforms and related display technologies.

Published

2019

28. Salmonella Typhi Porins OmpC and OmpF Are Potent Adjuvants for T-Dependent and T-Independent Antigens

Author

Marisol Pérez-Toledo, Nuriban Valero-Pacheco, Rodolfo Pastelin-Palacios, Cristina Gil-Cruz, Christian Perez-Shibayama, Mario A. Moreno-Eutimio, Ingeborg Becker, Sonia Mayra Pérez-Tapia, Lourdes Arriaga-Pizano, Adam F. Cunningham, Armando Isibasi, Laura C. Bonifaz, and Constantino López-Macías

Subjects

porins, adjuvants, influenza, Vi polysaccharide, IFN-gamma, IL-17, Immunologic diseases. Allergy, RC581-607

Abstract

Several microbial components, such as bacterial DNA and flagellin, have been used as experimental vaccine adjuvants because of their inherent capacity to efficiently activate innate immune responses. Likewise, our previous work has shown that the major Salmonella Typhi (S. Typhi) outer membrane proteins OmpC and OmpF (porins) are highly immunogenic protective antigens that efficiently stimulate innate and adaptive immune responses in the absence of exogenous adjuvants. Moreover, S. Typhi porins induce the expression of costimulatory molecules on antigen-presenting cells through toll-like receptor canonical signaling pathways. However, the potential of major S. Typhi porins to be used as vaccine adjuvants remains unknown. Here, we evaluated the adjuvant properties of S. Typhi porins against a range of experimental and clinically relevant antigens. Co-immunization of S. Typhi porins with ovalbumin (OVA), an otherwise poorly immunogenic antigen, enhanced anti-OVA IgG titers, antibody class switching, and affinity maturation. This adjuvant effect was dependent on CD4+ T-cell cooperation and was associated with an increase in IFN-γ, IL-17A, and IL-2 production by OVA-specific CD4+ T cells. Furthermore, co-immunization of S. Typhi porins with an inactivated H1N1 2009 pandemic influenza virus experimental vaccine elicited higher hemagglutinating anti-influenza IgG titers, antibody class switching, and affinity maturation. Unexpectedly, co-administration of S. Typhi porins with purified, unconjugated Vi capsular polysaccharide vaccine (Vi CPS)—a T-independent antigen—induced higher IgG antibody titers and class switching. Together, our results suggest that S. Typhi porins OmpC and OmpF are versatile vaccine adjuvants, which could be used to enhance T-cell immune responses toward a Th1/Th17 profile, while improving antibody responses to otherwise poorly immunogenic T-dependent and T-independent antigens.

Published

2017

29. Estrous cycle and gestational age-dependent expression of members of the interleukin-36 subfamily in a semi-allogeneic model of infected and non-infected murine pregnancy

Author

José Martin Murrieta Coxca, Fernando Gómez-Chávez, Damariz Adriana Baeza-Martínez, Mario Eugenio Cancino-Díaz, Juan Carlos Cancino-Díaz, Sonia Mayra Pérez-Tapia, Elba Reyes-Maldonado, and Sandra Rodríguez-Martínez

Subjects

Estrous Cycle, Inflammation, Listeria monocytogenes, Pregnancy Complications, Infectious, IL-36, Immunologic diseases. Allergy, RC581-607

Abstract

The IL-36 subfamily is a recently described group of cytokines with pro-inflammatory behavior, comprising three agonists (α, β and γ), its receptor (R) and one antagonist (Ra). The expression and function of IL-36 subfamily members in the estrous cycle in healthy and infected pregnancy have not been described. We evaluated mRNA and protein expression of IL-36 family members during the estrous cycle, implantation, fetal development and post-labor periods in a model of allogenic pregnancy in mice. We also explored the ability of Listeria monocytogenes to modulate expression of IL-36 subfamily members during pregnancy. Expression of IL-36 subfamily members showed different expression during the estrous cycle and pregnancy, but was induced at estrous, 16.5 days post coitum (dpc), 18.5 dpc and labor. IL-36 subfamily members showed a characteristic distribution in the glandular epithelium, perimetrium, myometrium, and stratum vasculare. Infection with Listeria monocytogenes during pregnancy induced strong production of IL-36 subfamily members, an observation that correlated with an increasing prevalence of fetal loss. Conclusions: IL-36 agonists showed specific patterns of mRNA and protein expression that might suggest functional specialization or specific target cells. Infection with Listeria monocytogenes during pregnancy induced strong production of IL-36 subfamily members.

Published

2016

30. Early Differentiation of Human CD11c+NK Cells with γδ T Cell Activation Properties Is Promoted by Dialyzable Leukocyte Extracts

Author

Dalia Ramírez-Ramírez, Eduardo Vadillo, Lourdes Andrea Arriaga-Pizano, Héctor Mayani, Sergio Estrada-Parra, Marco Antonio Velasco-Velázquez, Sonia Mayra Pérez-Tapia, and Rosana Pelayo

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

Reconstitution of the hematopoietic system during immune responses and immunological and neoplastic diseases or upon transplantation depends on the emergent differentiation of hematopoietic stem/progenitor cells within the bone marrow. Although in the last decade the use of dialyzable leukocyte extracts (DLE) as supportive therapy in both infectious and malignant settings has increased, its activity on the earliest stages of human hematopoietic development remains poorly understood. Here, we have examined the ability of DLE to promote replenishment of functional lymphoid lineages from CD34+ cells. Our findings suggest that DLE increases their differentiation toward a conspicuous CD56+CD16+CD11c+ NK-like cell population endowed with properties such as IFNy production, tumor cell cytotoxicity, and the capability of inducing γδ T lymphocyte proliferation. Of note, long-term coculture controlled systems showed the bystander effect of DLE-stromal cells by providing NK progenitors with signals to overproduce this cell subset. Thus, by direct effect on progenitor cells and through activation and remodeling of the supporting hematopoietic microenvironment, DLE may contribute a robust innate immune response by promoting the emerging lymphopoiesis of functional CD11c+ NK cells in a partially TLR-related manner. Unraveling the identity and mechanisms of the involved DLE components may be fundamental to advance the NK cell-based therapy field.

Published

2016

31. Herpes Murine Model as a Biological Assay to Test Dialyzable Leukocyte Extracts Activity

Author

Nohemí Salinas-Jazmín, Sergio Estrada-Parra, Miguel Angel Becerril-García, Alberto Yairh Limón-Flores, Said Vázquez-Leyva, Emilio Medina-Rivero, Lenin Pavón, Marco Antonio Velasco-Velázquez, and Sonia Mayra Pérez-Tapia

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

Human dialyzable leukocyte extracts (DLEs) are heterogeneous mixtures of low-molecular-weight peptides that are released on disruption of peripheral blood leukocytes from healthy donors. DLEs improve clinical responses in infections, allergies, cancer, and immunodeficiencies. Transferon is a human DLE that has been registered as a hemoderivate by Mexican health authorities and commercialized nationally. To develop an animal model that could be used routinely as a quality control assay for Transferon, we standardized and validated a murine model of cutaneous HSV-1 infection. Using this model, we evaluated the activity of 27 Transferon batches. All batches improved the survival of HSV-1-infected mice, wherein average survival rose from 20.9% in control mice to 59.6% in Transferon-treated mice. The activity of Transferon correlated with increased serum levels of IFN-γ and reduced IL-6 and TNF-α concentrations. Our results demonstrate that (i) this mouse model of cutaneous herpes can be used to examine the activity of DLEs, such as Transferon; (ii) the assay can be used as a routine test for batch release; (iii) Transferon is produced with high homogeneity between batches; (iv) Transferon does not have direct virucidal, cytoprotective, or antireplicative effects; and (v) the protective effect of Transferon in vivo correlates with changes in serum cytokines.

Published

2015

32. Evidence that cervical cancer cells cultured as tumorspheres maintain high CD73 expression and increase their protumor characteristics through TGF‐β production

Author

Rosario García‐Rocha, Alberto Monroy‐García, Monserrat Carrera‐Martínez, Jorge Hernández‐Montes, Christian Azucena Don‐López, Benny Weiss‐Steider, Katia Alhelí Monroy‐Mora, María de los Ángeles Ponce‐Chavero, Juan José Montesinos‐Montesinos, María Luisa Escobar‐Sánchez, Gabriela Molina Castillo, Rommel Chacón‐Salinas, Luis Vallejo‐Castillo, Sonia Mayra Pérez‐Tapia, and María de Lourdes Mora‐García

Subjects

Clinical Biochemistry, Cell Biology, General Medicine, Biochemistry

Published

2022

33. IL-6, IL-10, sFas, granulysin and indicators of intestinal permeability as early biomarkers for a fatal outcome in COVID-19

Author

Alejandro Hernández-Solis, Azmavet M. Güemes-González, Ximena Ruiz-Gómez, Pablo Álvarez-Maldonado, Jessica Castañeda-Casimiro, Argelia Flores-López, Martha Alicia Ramírez-Guerra, Omar Muñoz-Miranda, Ruth L. Madera-Sandoval, Lourdes A. Arriaga-Pizano, Alejandro Nieto-Patlán, Sergio Estrada-Parra, Sonia Mayra Pérez-Tapia, Jeanet Serafín-López, Rommel Chacón-Salinas, Alejandro Escobar-Gutiérrez, Rodolfo Soria-Castro, Bibiana Patricia Ruiz-Sánchez, and Isabel Wong-Baeza

Subjects

Intestines, SARS-CoV-2, Interleukin-6, Coinfection, Sepsis, Immunology, Immunology and Allergy, Humans, COVID-19, Hematology, Permeability, Biomarkers, Interleukin-10

Abstract

The clinical presentation of coronavirus disease 2019 (COVID-19), which is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), ranges between mild respiratory symptoms and a severe disease that shares many of the features of sepsis. Sepsis is a deregulated response to infection that causes life-threatening organ failure. During sepsis, the intestinal epithelial cells are affected, causing an increase in intestinal permeability and allowing microbial translocation from the intestine to the circulation, which exacerbates the inflammatory response. Here we studied patients with moderate, severe and critical COVID-19 by measuring a panel of molecules representative of the innate and adaptive immune responses to SARS-CoV-2, which also reflect the presence of systemic inflammation and the state of the intestinal barrier. We found that non-surviving COVID-19 patients had higher levels of low-affinity anti-RBD IgA antibodies than surviving patients, which may be a response to increased microbial translocation. We identified sFas and granulysin, in addition to IL-6 and IL-10, as possible early biomarkers with high sensitivity (73 %) and specificity (51 %) to discriminate between surviving and non-surviving COVID-19 patients. Finally, we found that the microbial metabolite d-lactate and the tight junction regulator zonulin were increased in the serum of patients with severe COVID-19 and in COVID-19 patients with secondary infections, suggesting that increased intestinal permeability may be a source of secondary infections in these patients. COVID-19 patients with secondary infections had higher disease severity and mortality than patients without these infections, indicating that intestinal permeability markers could provide complementary information to the serum cytokines for the early identification of COVID-19 patients with a high risk of a fatal outcome.

Published

2022

34. Quality attributes of partially hydrolyzed collagen in a liquid formulation used for skin care

Author

Marco A. Velasco-Velázquez, Lenin Pavón, Pamela G. Merlos Rivera, José Enrique Herbert-Pucheta, Daniel Montoya‐Escutia, Carlos A. López-Morales, Said Vázquez-Leyva, Luis Gerardo Zepeda-Vallejo, Ignacio Mejía-Calvo, Emilio Medina-Rivero, Leonardo E. López‐Juárez, and Sonia Mayra Pérez-Tapia

Subjects

Skin Care Articles, safety cosmetic product, Facial rejuvenation, liquid formulation, hydrolyzed collagen, Dermatology, quality attributes cosmetic, Skin Aging, 030207 dermatology & venereal diseases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Humans, Rejuvenation, Thermal stability, Hydrolyzed collagen, skin aging, Protein secondary structure, Skin, Chromatography, Molecular mass, Chemistry, Hypoallergenic, Original Contribution, Skin Care, 030220 oncology & carcinogenesis, Collagen, Triple helix

Abstract

Background The deterioration of the skin accentuates over time, affecting its aesthetic appearance. This is characterized by the weakening of the mechanisms involved in the regeneration and repair of the dermal matrix. Consequently, the skin losses elasticity and smoothness resulting in the formation of wrinkles. The alternatives for facial rejuvenation include surgery, injection of botulinum toxin, and the application of masks. Topic products are less invasive, can be self‐applied, and have an increased benefit/risk relationship. Aim We developed a liquid formulation containing collagen hydrolyzed and evaluated the product by cutting‐edge technology in order to define proper its quality attributes. Methods We employed nuclear magnetic resonance (NMR), size‐exclusion chromatography (SEC), and mass spectrometry (MS). Additionally, we analyzed its cosmetical effect in five volunteers and we demonstrate the product safety. Results Our results demonstrate the following: (a) a stable secondary structure identity associated to the known triple helix arrangement in liquid and solid states; (b) a typical conformational flexibility depending on its hydration state; (c) thermal stability confirmed by liquid‐ and solid‐state nuclear magnetic resonance schemes; and (d) a molecular mass distribution of peptides between 0.5 and 19.5 kDa. The product faded wrinkles in the forehead, an effect that remained after removing the mask. The formula was non‐irritating and hypoallergenic. Conclusion We characterized, using state‐of‐the‐art methodologies, the quality attributes that are critical for the safety and beneficial effect of a new collagen‐containing formula.

Published

2020

35. Pranlukast Antagonizes CD49f and Reduces Stemness in Triple-Negative Breast Cancer Cells

Author

Fabiola Cortés-Mendoza, Diana Casique-Aguirre, Carlos A. García-Pérez, Sonia Mayra Pérez-Tapia, Aliesha González-Arenas, Inés Velázquez-Quesada, Marisol de la Fuente-Granada, Charmina Aguirre-Alvarado, Angel J Ruiz-Moreno, Aldo Segura-Cabrera, and Marco A. Velasco-Velázquez

Subjects

0301 basic medicine, Pharmacology, biology, Chemistry, CD44, Pharmaceutical Science, Cancer, medicine.disease, Pranlukast, 03 medical and health sciences, Transactivation, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Drug Discovery, Cancer research, medicine, biology.protein, Viability assay, Stem cell, Cell adhesion, Triple-negative breast cancer, medicine.drug

Abstract

Introduction Cancer stem cells (CSCs) drive the initiation, maintenance, and therapy response of breast tumors. CD49f is expressed in breast CSCs and functions in the maintenance of stemness. Thus, blockade of CD49f is a potential therapeutic approach for targeting breast CSCs. In the present study, we aimed to repurpose drugs as CD49f antagonists. Materials and methods We performed consensus molecular docking using a subdomain of CD49f that is critical for heterodimerization and a collection of pharmochemicals clinically tested. Molecular dynamics simulations were employed to further characterize drug-target binding. Using MDA-MB-231 cells, we evaluated the effects of potential CD49f antagonists on 1) cell adhesion to laminin; 2) mammosphere formation; and 3) cell viability. We analyzed the effects of the drug with better CSC-selectivity on the activation of CD49f-downstream signaling by Western blot (WB) and co-immunoprecipitation. Expressions of the stem cell markers CD44 and SOX2 were analyzed by flow cytometry and WB, respectively. Transactivation of SOX2 promoter was evaluated by luciferase reporter assays. Changes in the number of CSCs were assessed by limiting-dilution xenotransplantation. Results Pranlukast, a drug used to treat asthma, bound to CD49f in silico and inhibited the adhesion of CD49f+ MDA-MB-231 cells to laminin, indicating that it antagonizes CD49f-containing integrins. Molecular dynamics analysis showed that pranlukast binding induces conformational changes in CD49f that affect its interaction with β1-integrin subunit and constrained the conformational dynamics of the heterodimer. Pranlukast decreased the clonogenicity of breast cancer cells on mammosphere formation assay but had no impact on the viability of bulk tumor cells. Brief exposure of MDA-MB-231 cells to pranlukast altered CD49f-dependent signaling, reducing focal adhesion kinase (FAK) and phosphatidylinositol 3-kinase (PI3K) activation. Further, pranlukast-treated cells showed decreased CD44 and SOX2 expression, SOX2 promoter transactivation, and in vivo tumorigenicity, supporting that this drug reduces the frequency of CSC. Conclusion Our results support the function of pranlukast as a CD49f antagonist that reduces the CSC population in triple-negative breast cancer cells. The pharmacokinetics and toxicology of this drug have already been established, rendering a potential adjuvant therapy for breast cancer patients.

Published

2020

36. COVID-19 relevant genetic variants confirmed in an admixed population

Author

Tomas Texis, José Luis Cruz-Jaramilllo, Willebaldo García-Muñoz, Lourdes Anzures-Cortés, Lorenza Haddad-Talancón, Sergio Sánchez-García, María del Carmen Jiménez Martínez, Edgar Pérez Barragán, Alejandro Nieto-Patlán, José D. Martínez-Ezquerro, Kenneth Rubio-Carrasco, Mauricio Rodríguez-Dorantes, Sergio Cortés-Ramírez, Gabriela Mellado-Sánchez, Sonia Mayra Pérez-Tapia, and Vanessa Gonzalez-Covarrubias

Abstract

SummaryThe dissection of factors that contribute to COVID-19 infection and severity has overwhelmed the scientific community for almost 2 years. Current reports highlight the role of in disease incidence, progression, and severity. Here, we aimed to confirm the presence of previously reported genetic variants in an admixed population. Allele frequencies were assessed and compared between the general population (N=3079) for which at least 30% have not been infected with SARS-CoV2 as per July 2021 versus COVID-19 patients (N=106).Genotyping data from the Illumina GSA array was used to impute genetic variation for 14 COVID-relevant genes, using the 1000G phase 3 as reference based on the human genome assembly hg19, following current standard protocols and recommendations for genetic imputation. Bioinformatic and statistical analyses were performed using MACH v1.0, R, and PLINK.A total of 7953 variants were imputed on, ABO, CCR2, CCR9, CXCR6, DPP9, FYCO1, IL10RB/IFNAR2, LZTFL1, OAS1, OAS2, OAS3, SLC6A20, TYK2, and XCR1. Statistically significant allele differences were reported for 10 and 7 previously identified and confirmed variants, ABO rs657152, DPP9 rs2109069, LZTFL1 rs11385942, OAS1 rs10774671, OAS1 rs2660, OAS2 rs1293767, and OAS3 rs1859330 pOur observations confirm the presence of genetic differences in COVID-19 patients in an admixed population and prompts for the investigation of the statistical relevance of additional variants on these and other genes that could identify local and geographical patterns of COVID-19.

Published

2022

37. Structural and Physicochemical Characteristics of One-Step PAMAM Dendrimeric Nanoparticles

Author

Eva Ramón-Gallegos, Childérick Séverac, Said Vázquez-Leyva, Sergio Andrés Torres-Pérez, Luis Vallejo-Castillo, José Enrique Herbert-Pucheta, Etienne Dague, Luis Gerardo Zepeda-Vallejo, Sonia Mayra Pérez-Tapia, Instituto Politecnico Nacional [Mexico] (IPN), Institut des Technologies Avancées en sciences du Vivant (ITAV), Université Toulouse III - Paul Sabatier (UT3), Université de Toulouse (UT)-Université de Toulouse (UT)-Centre National de la Recherche Scientifique (CNRS), Équipe Ingénierie pour les sciences du vivant (LAAS-ELIA), Laboratoire d'analyse et d'architecture des systèmes (LAAS), Université Toulouse Capitole (UT Capitole), Université de Toulouse (UT)-Université de Toulouse (UT)-Institut National des Sciences Appliquées - Toulouse (INSA Toulouse), Institut National des Sciences Appliquées (INSA)-Université de Toulouse (UT)-Institut National des Sciences Appliquées (INSA)-Université Toulouse - Jean Jaurès (UT2J), Université de Toulouse (UT)-Université Toulouse III - Paul Sabatier (UT3), Université de Toulouse (UT)-Centre National de la Recherche Scientifique (CNRS)-Institut National Polytechnique (Toulouse) (Toulouse INP), Université de Toulouse (UT)-Université Toulouse Capitole (UT Capitole), and Université de Toulouse (UT)

Subjects

Materials science, Atomic force microscopy, Poly(amidoamine), Dispersity, Amidoamine, Nanoparticle, One-Step, Nanotechnology, orthogonal polydispersity index, PFG-DOSY NMR, Molecular Weight, [CHIM.THEO]Chemical Sciences/Theoretical and/or physical chemistry, chemistry.chemical_compound, Colloid and Surface Chemistry, [CHIM.POLY]Chemical Sciences/Polymers, chemistry, Dendrimer, Zeta potential, Nanocarriers

Abstract

The recently developed One-Step Poly(amidoamine) (OS-PAMAM) dendrimers stand out for their characteristics as the high drug-load capacity and cell-delivery improvement of therapeutic agents. The OS-PAMAM dendrimers have proven to be useful in the biomedical field as nanocarrier or nanosystems for therapy. In the present research it was encouraging to determine their physicochemical characteristics which were compared with commercial PAMAM generation-6 (G6). The spectroscopic measurement of amides, nanoparticle size (10–30 nm), polydispersity index and zeta potential measurements correlates with the commercial product. The OS-PAMAM has cavities detected by AFM, and the force analysis showed the same adhesion force and different elasticity than PAMAM-G6. The molecular weight (MW) was 10 times lower than the commercial one for both techniques employed, resembling the MW of a PAMAM generation-3 (G3). OS-PAMAM/PAMAM-G6 MS-MS mirror plots demonstrate chemical equivalency amongst herein analyzed dendrimers, with the advantage that OS-PAMAM is produced with a faster and low-cost synthetic protocol, which allows them to be applied for both research and industry in the biomedical field.

Published

2022

38. Patient-Derived Bone Marrow Spheroids Reveal Leukemia-Initiating Cells Supported by Mesenchymal Hypoxic Niches in Pediatric B-ALL

Author

Sonia Mayra Pérez-Tapia, Erick Armenta-Castro, Vianney Ortiz-Navarrete, Jose Davila-Velderrain, Lilia Adela García-Stivalet, Aurora Rodríguez-Martínez, Rosana Pelayo, Vanessa Terán-Cerqueda, Monica L. Guzman, Antonio Sandoval-Cabrera, Duane C. Hassane, Bertha Alicia León-Chávez, Verónica Vallejo-Ruiz, Gabriela Zamora-Herrera, José Alejandro Limón-Flores, and Juan Carlos Balandrán

Subjects

Population, Immunology, acute lymphoblastic leukemia, Biology, bone marrow niche, Mice, Bone Marrow, Spheroids, Cellular, medicine, Tumor Cells, Cultured, Immunology and Allergy, Animals, Humans, leukemia-initiating cell, tumor microenvironment, Lymphopoiesis, Stem Cell Niche, education, Original Research, education.field_of_study, Tumor microenvironment, B-cell development, Mesenchymal stem cell, Mesenchymal Stem Cells, Precursor Cell Lymphoblastic Leukemia-Lymphoma, RC581-607, medicine.disease, Leukemia, Haematopoiesis, medicine.anatomical_structure, Cancer research, Neoplastic Stem Cells, Heterografts, Female, Bone marrow, Stem cell, Immunologic diseases. Allergy, mesenchymal stromal cells

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) results from the expansion of malignant lymphoid precursors within the bone marrow (BM), where hematopoietic niches and microenvironmental signals provide leukemia-initiating cells (LICs) the conditions to survive, proliferate, initiate disease, and relapse. Normal and malignant lymphopoiesis are highly dependent on the BM microenvironment, particularly on CXCL12-abundant Reticular (CAR) cells, which provide a niche for maintenance of primitive cells. During B-ALL, leukemic cells hijack BM niches, creating a proinflammatory milieu incompetent to support normal hematopoiesis but favoring leukemic proliferation. Although the lack of a phenotypic stem cell hierarchy is apparent in B-ALL, LICs are a rare and quiescent population potentially responsible for chemoresistance and relapse. Here, we developed novel patient-derived leukemia spheroids (PDLS), an ex vivo avatar model, from mesenchymal stromal cells (MSCs) and primary B-ALL cells, to mimic specialized niche structures and cell-to-cell intercommunication promoting normal and malignant hematopoiesis in pediatric B-ALL. 3D MSC spheroids can recapitulate CAR niche-like hypoxic structures that produce high levels of CXCL10 and CXCL11. We found that PDLS were preferentially enriched with leukemia cells displaying functional properties of LICs, such as quiescence, low reactive oxygen species, drug resistance, high engraftment in immunodeficient mice, and long-term leukemogenesis. Moreover, the combination of PDLS and patient-derived xenografts confirmed a microenvironment-driven hierarchy in their leukemic potential. Importantly, transcriptional profiles of MSC derived from primary patient samples revealed two unique signatures (1), a CXCL12low inflammatory and leukemia expansion (ILE)-like niche, that likely supports leukemic burden, and (2) a CXCL11hi immune-suppressive and leukemia-initiating cell (SLIC)-like niche, where LICs are likely sustained. Interestingly, the CXCL11+ hypoxic zones were recapitulated within the PDLS that are capable of supporting LIC functions. Taken together, we have implemented a novel PDLS system that enriches and supports leukemia cells with stem cell features driven by CXCL11+ MSCs within hypoxic microenvironments capable of recapitulating key features, such as tumor reemergence after exposure to chemotherapy and tumor initiation. This system represents a unique opportunity for designing ex vivo personalized avatars for B-ALL patients to evaluate their own LIC pathobiology and drug sensitivity in the context of the tumor microenvironment.

Published

2021

39. Identity Profiling of Complex Mixtures of Peptide Products by Structural and Mass Mobility Orthogonal Analysis

Author

Lenin Pavón, Carlos A. López-Morales, L. Gerardo Zepeda-Vallejo, Emilio Medina-Rivero, Said Vázquez-Leyva, Sonia Mayra Pérez-Tapia, Marco A. Velasco-Velázquez, Luis Vallejo-Castillo, and José Enrique Herbert-Pucheta

Subjects

chemistry.chemical_classification, Magnetic Resonance Spectroscopy, Hydrolysis, 010401 analytical chemistry, Peptide, Glatiramer Acetate, Computational biology, 010402 general chemistry, 01 natural sciences, Mass Spectrometry, 0104 chemical sciences, Analytical Chemistry, Molecular Weight, chemistry, Leukocytes, Critical to quality, Humans, Profiling (information science), Collagen, Immunosuppressive Agents

Abstract

Identity is a critical quality attribute that must be determined before releasing batches of medicinal and dietary products. However, the identities of peptide-derived products composed of a large number of diverse molecules is challenging since most analytical techniques cannot analyze multiple molecules simultaneously. Here, we proposed the determination of the weight-average molecular weight (

Published

2019

40. Targeting Breast Cancer Stem Cells: A Methodological Perspective

Author

Inés Velázquez-Quesada, Sonia Mayra Pérez-Tapia, Marco A. Velasco-Velázquez, and Luz X. Vásquez-Bochm

Subjects

business.industry, Medicine (miscellaneous), Antineoplastic Agents, Breast Neoplasms, Tumor cells, General Medicine, Self renewal, medicine.disease, Tumor heterogeneity, Breast cancer, Cancer stem cell, Biological property, Neoplastic Stem Cells, Cancer research, Animals, Humans, Medicine, Female, Experimental methods, Stem cell, business

Abstract

Cancer Stem Cells (CSCs) constitute a subpopulation at the top of the tumor cell hierarchy that contributes to tumor heterogeneity and is uniquely capable of seeding new tumors. Because of their biological properties, CSCs have been pointed out as therapeutic targets for the development of new therapies against breast cancer. The identification of drugs that selectively target breast CSCs requires a clear understanding of their biological functions and the experimental methods to evaluate such hallmarks. Herein, we review the methods to study breast CSCs properties and discuss their value in the preclinical evaluation of CSC-targeting drugs.

Published

2019

41. Transcriptome-based identification of lovastatin as a breast cancer stem cell-targeting drug

Author

Aliesha González-Arenas, Sonia Mayra Pérez-Tapia, Mireya Velázquez-Paniagua, Sandra L. Guerrero-Rodríguez, Luz X. Vásquez-Bochm, Sandra S. Castro-Vázquez, Marco A. Velasco-Velázquez, Abimael Mondragon-Peralta, and Marisol de la Fuente-Granada

Subjects

Transcriptional Activation, Down-Regulation, Breast Neoplasms, Transcriptome, Mice, 03 medical and health sciences, Transactivation, Drug Delivery Systems, 0302 clinical medicine, Breast cancer, SOX2, Cell Line, Tumor, Animals, Humans, Medicine, MTT assay, Lovastatin, Promoter Regions, Genetic, Pharmacology, business.industry, SOXB1 Transcription Factors, General Medicine, medicine.disease, Drug repositioning, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, Cancer research, Female, lipids (amino acids, peptides, and proteins), Neoplasm Recurrence, Local, Stem cell, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Background Breast cancer is a neoplastic disease with high morbidity and mortality in women worldwide. Breast cancer stem cells (CSCs) have a significant function in tumor growth, recurrence, and therapeutic resistance. Thus, CSCs have been pointed as targets of new therapies for breast cancer. Herein, we aimed to repurpose certain drugs as breast CSC-targeting agents. Methods We compared a consensus breast CSC signature with the transcriptomic changes that were induced by over 1300 bioactive compounds using Connectivity Map. The effects of the selected drugs on SOX2 promoter transactivation, SOX2 expression, viability, clonogenicity, and ALDH activity in breast cancer cells were analyzed by luciferase assay, western blot, MTT assay, mammosphere formation assay, and ALDEFLUOR® test, respectively. Gene Set Enrichment Analysis (GSEA) was performed using the gene expression data from mammary tumors of mice that were treated with lovastatin. Results Five drugs (fasudil, pivmecillinam, ursolic acid, 16,16-dimethylprostaglandin E2, and lovastatin) induced signatures that correlated negatively with the query CSC signature. In vitro, lovastatin inhibited SOX2 promoter transactivation, and reduced the efficiency of mammosphere formation and the percentage of ALDH+ cells. Mevalonate mitigated the effects of lovastatin, suggesting that the targeting of CSCs by lovastatin was mediated by the inhibition of its reported target, 3-hydroxy-3-methyl-glutaryl-coenzyme A reductase (HMGCR). By GSEA, lovastatin downregulated genes that are involved in stemness and invasiveness in mammary tumors, corroborating our in vitro findings. Conclusion Lovastatin is a breast CSC-targeting drug. The inhibition of HMGCR might develop new adjuvant therapeutic strategies for breast tumors.

Published

2019

42. Development and Evaluation of a Set of Spike and Receptor Binding Domain-Based Enzyme-Linked Immunosorbent Assays for SARS-CoV-2 Serological Testing

Author

Gregorio Carballo-Uicab, Juan Carlos Almagro, Gabriela Medina, Laura Montiel-Cervantes, Alejandro Nieto-Patlán, Luis Vallejo-Castillo, Irma López-Martínez, Alejandra Montes-Luna, Maria C. Jiménez-Martínez, Roberto Vázquez-Campuzano, Keyla M. Gómez-Castellano, Hugo Iván Arrieta-Oliva, Rosa Camacho-Sandoval, Edith González-González, Omar U. Guzmán-Bringas, María Pilar Cruz-Domínguez, Sonia Mayra Pérez-Tapia, Belem Torres-Longoria, and Maricela Gordillo-Marín

Subjects

Medicine (General), Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Clinical Biochemistry, Article, Serology, R5-920, Medicine, Seroconversion, seroconversion, chemistry.chemical_classification, UDITEST-V2G®, biology, business.industry, COVID-19, IgG isotypes, Virology, Isotype, Primary and secondary antibodies, Titer, Enzyme, chemistry, biology.protein, serological diagnostics, business

Abstract

The implementation and validation of anti-SARS-CoV-2 IgG serological assays are reported in this paper. S1 and RBD proteins were used to coat ELISA plates, and several secondary antibodies served as reporters. The assays were initially validated with 50 RT-PCR positive COVID-19 sera, which showed high IgG titers of mainly IgG1 isotype, followed by IgG3. Low or no IgG2 and IgG4 titers were detected. Then, the RBD/IgG assay was further validated with 887 serum samples from RT-PCR positive COVID-19 individuals collected at different times, including 7, 14, 21, and 40 days after the onset of symptoms. Most of the sera were IgG positive at day 40, with seroconversion happening after 14–21 days. A third party conducted an additional performance test of the RBD/IgG assay with 406 sera, including 149 RT-PCR positive COVID-19 samples, 229 RT-PCR negative COVID-19 individuals, and 28 sera from individuals with other viral infections not related to SARS-CoV-2. The sensitivity of the assay was 99.33%, with a specificity of 97.82%. All the sera collected from individuals with infectious diseases other than COVID-19 were negative. Given the robustness of this RBD/IgG assay, it received approval from the sanitary authority in Mexico (COFEPRIS) for production and commercialization under the name UDISTEST-V2G®.

Published

2021

43. Severe COVID-19 is marked by dysregulated serum levels of carboxypeptidase A3 and serotonin

Author

José L. Maravillas-Montero, Diana Gómez-Martín, Sergio Estrada-Parra, Marcia Campillo-Navarro, Gloria M. Rodríguez-López, Alfredo Pérez-Fragoso, Rodolfo Soria-Castro, Alma Chavez-Blanco, Yatsiri G Meneses-Preza, Rodrigo Cervantes-Díaz, Rommel Chacón-Salinas, Violeta D. Álvarez-Jiménez, Víctor A. Sosa-Hernandez, José J. Torres-Ruíz, Sandra Romero-Ramírez, and Sonia Mayra Pérez-Tapia

Subjects

0301 basic medicine, ARDS, CPA3, Serotonin, Carboxypeptidases A, Immunology, Inflammation, Biology, Severity of Illness Index, SARS‐CoV‐2, Proinflammatory cytokine, Mast cell, 03 medical and health sciences, 0302 clinical medicine, Immune system, carboxypeptidase A3, COVID‐19, Immunology and Allergy, Medicine, Humans, Mast Cells, B cell, Innate immune system, business.industry, SARS-CoV-2, COVID-19, Cell Biology, medicine.disease, Pathophysiology, 030104 developmental biology, medicine.anatomical_structure, Highlighted Article, 030220 oncology & carcinogenesis, medicine.symptom, Inflammation Mediators, business, Biomarkers, Respiratory tract

Abstract

The immune response plays a critical role in the pathophysiology of SARS‐CoV‐2 infection ranging from protection to tissue damage and all occur in the development of acute respiratory distress syndrome (ARDS). ARDS patients display elevated levels of inflammatory cytokines and innate immune cells, and T and B cell lymphocytes have been implicated in this dysregulated immune response. Mast cells are abundant resident cells of the respiratory tract and are able to release different inflammatory mediators rapidly following stimulation. Recently, mast cells have been associated with tissue damage during viral infections, but their role in SARS‐CoV‐2 infection remains unclear. In this study, we examined the profile of mast cell activation markers in the serum of COVID‐19 patients. We noticed that SARS‐CoV‐2‐infected patients showed increased carboxypeptidase A3 (CPA3) and decreased serotonin levels in their serum when compared with symptomatic SARS‐CoV‐2‐negative patients. CPA3 levels correlated with C‐reactive protein, the number of circulating neutrophils, and quick SOFA. CPA3 in serum was a good biomarker for identifying severe COVID‐19 patients, whereas serotonin was a good predictor of SARS‐CoV‐2 infection. In summary, our results show that serum CPA3 and serotonin levels are relevant biomarkers during SARS‐CoV‐2 infection. This suggests that mast cells and basophils are relevant players in the inflammatory response in COVID‐19 and may represent targets for therapeutic intervention., Graphical Abstract Serum levels of CPA3 and serotonin are affected during SARS‐CoV‐2 infection and can be considered as biomarkers during COVID‐19.

Published

2021

44. Poor Survival in COVID-19 Associated with Lymphopenia and Higher Neutrophile-Lymphocyte Ratio

Author

Laura A, Montiel-Cervantes, Gabriela, Medina, Maria, Pilar Cruz-Domínguez, Sonia-Mayra, Pérez-Tapia, Maria C, Jiménez-Martínez, Hugo-Iván, Arrieta-Oliva, Gregorio, Carballo-Uicab, Laura, López-Pelcastre, and Rosa, Camacho-Sandoval

Subjects

CD4-Positive T-Lymphocytes, Male, Neutrophils, COVID-19, Kaplan-Meier Estimate, CD8-Positive T-Lymphocytes, Middle Aged, Killer Cells, Natural, Leukocyte Count, Cross-Sectional Studies, Predictive Value of Tests, Lymphopenia, Humans, Female, Mortality, Symptom Assessment, Correlation of Data, Mexico, Biomarkers

Abstract

Immune cell counts in blood in severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) infection may be useful prognostic biomarkers of disease severity, mortality, and response to treatment.To analyze sub-populations of lymphocytes at hospital admission in survivors and deceased from severe pneumonia due to coronavirus disease-2019 (COVID-19).We conducted a cross-sectional study of healthcare workers confirmed with SARS-CoV-2 in convalescents (control group) and healthy controls (HC) diagnosed with severe COVID-19. Serum samples were taken at hospital admission and after recovery. Serum samples ≥ 25 days after onset of symptoms were analyzed for lymphocyte subpopulations through flow cytometry. Descriptive statistics, Kruskall-Wallis test, receiver operating characteristic curve, calculation of sensitivity, specificity, predictive values, and Kaplan-Meier analysis were performed.We included 337 patients: 120 HC, 127 convalescents, and 90 severe COVID-19 disease patients (50 survivors, 40 deceased). For T cells, total lymphocytes ≥ 800/μL, CD3+ ≥ 400/μL, CD4+ ≥ 180/μL, CD8+ ≥ 150/μL, B cells CD19+ ≥ 80/μL, and NK ≥ 34/μL subsets were associated with survival in severe COVID-19 disease patients. All subtypes of lymphocytes had higher concentrations in survivors than deceased, but similar between HC and convalescents. Leukocytes ≥ 10.150/μL or neutrophils ≥ 10,000/μL were associated with increased mortality. The neutrophil-to-lymphocyte ratio (NLR) ≥ 8.5 increased the probability of death in severe COVID-19 (odds ratio 11.68).Total lymphocytes; NLR; and levels of CD3+, CD4+, CD8+, and NK cells are useful as biomarkers of survival or mortality in severe COVID-19 disease and commonly reach normal levels in convalescents.

Published

2021

45. LPA

Author

Silvia Anahi Valdés-Rives, Olga Villamar-Cruz, Luis E. Arias-Romero, Carmen J. Zamora-Sánchez, Sonia Mayra Pérez-Tapia, Ignacio Camacho-Arroyo, Aliesha González-Arenas, Denisse Arcos-Montoya, and Marisol de la Fuente-Granada

Subjects

Vascular Endothelial Growth Factor A, Protein Kinase C-alpha, LPA1 receptor, Article, progesterone receptor, chemistry.chemical_compound, Phosphoserine, Cell Movement, Cell Line, Tumor, Lysophosphatidic acid, Progesterone receptor, Humans, RNA, Messenger, Phosphorylation, Receptors, Lysophosphatidic Acid, Promoter Regions, Genetic, lcsh:QH301-705.5, Protein kinase C, Cell Nucleus, LPAR1, Kinase, Brain Neoplasms, Phosphoric Diester Hydrolases, General Medicine, Survival Analysis, nervous system diseases, ErbB Receptors, Gene Expression Regulation, Neoplastic, Protein Transport, lcsh:Biology (General), chemistry, Cancer research, protein kinase C α, lipids (amino acids, peptides, and proteins), Signal transduction, Lysophospholipids, Glioblastoma, Receptors, Progesterone, Intracellular, Protein Binding

Abstract

Lysophosphatidic acid (LPA) induces a wide range of cellular processes and its signaling is increased in several cancers including glioblastoma (GBM), a high-grade astrocytoma, which is the most common malignant brain tumor. LPA1 receptor is expressed in GBM cells and its signaling pathways activate protein kinases C (PKCs). A downstream target of PKC, involved in GBM progression, is the intracellular progesterone receptor (PR), which can be phosphorylated by this enzyme, increasing its transcriptional activity. Interestingly, in GBM cells, PKCα isotype translocates to the nucleus after LPA stimulation, resulting in an increase in PR phosphorylation. In this study, we determined that LPA1 receptor activation induces protein-protein interaction between PKCα and PR in human GBM cells, this interaction increased PR phosphorylation in serine400. Moreover, LPA treatment augmented VEGF transcription, a known PR target. This effect was blocked by the PR selective modulator RU486, also, the activation of LPA1/PR signaling promoted migration of GBM cells. Interestingly, using TCGA data base, we found that mRNA expression of LPAR1 increases according to tumor malignancy and correlates with a lower survival in grade III astrocytomas. These results suggest that LPA1/PR pathway regulates GBM progression.

Published

2021

46. Detection of CD39 and a Highly Glycosylated Isoform of Soluble CD73 in the Plasma of Patients with Cervical Cancer: Correlation with Disease Progression

Author

Luis Roberto Ávila-Ibarra, María de Lourdes Mora-García, Rosario García-Rocha, Daniela Berenice Torres-Pineda, Adriana Aguilar-Lemarroy, Sonia Mayra Pérez-Tapia, Gabriela Molina-Castillo, Luis Vallejo-Castillo, Ricardo Muñóz-Godínez, Juan José Montesinos-Montesinos, Benny Weiss-Steider, Jorge Hernández-Montes, Christian Azucena Don-López, Alberto Monroy-García, and Rommel Chacón-Salinas

Subjects

Adenosine monophosphate, Gene isoform, Adult, Article Subject, Immunology, Uterine Cervical Neoplasms, Enzyme-Linked Immunosorbent Assay, Endoglycosidase H, chemistry.chemical_compound, Antigens, CD, medicine, Pathology, RB1-214, Humans, 5'-Nucleotidase, Cervical cancer, biology, Apyrase, Cancer, Cell Biology, medicine.disease, Molecular biology, Adenosine, Adenosine Monophosphate, Adenosine Diphosphate, Adenosine diphosphate, chemistry, Concomitant, biology.protein, Female, medicine.drug, Research Article

Abstract

Persistent infection with high-risk human papillomavirus (HR-HPV) is the main factor in the development of cervical cancer (CC). The presence of immunosuppressive factors plays an important role in the development of this type of cancer. To determine whether CD39 and CD73, which participate in the production of immunosuppressive adenosine (Ado), are involved in the progression of CC, we compared the concentrations and hydrolytic activity of these ectonucleotidases in platelet-free plasma (PFP) samples between patients with low-grade squamous intraepithelial lesions (LSILs) ( n = 18 ), high-grade squamous intraepithelial lesions (HSILs) ( n = 12 ), and CC ( n = 19 ) and normal donors (NDs) ( n = 15 ). The concentrations of CD39 and CD73 in PFP increased with disease progression ( r = 0.5929 , p < 0.001 ). The PFP of patients with HSILs or CC showed the highest concentrations of CD39 (2.3 and 2.2 times that of the NDs, respectively) and CD73 (1.7 and 2.68 times that of the NDs, respectively), which were associated with a high capacity to generate Ado from the hydrolysis of adenosine diphosphate (ADP) and adenosine monophosphate (AMP). The addition of POM-1 and APCP, specific inhibitors of CD39 and CD73, respectively, inhibited the ADPase and AMPase activity of PFP by more than 90%. A high level of the 90 kD isoform of CD73 was detected in the PFP of patients with HSILs or CC. Digestion with endoglycosidase H and N-glycanase generated CD73 with weights of approximately 90 kD, 85 kD, 80 kD, and 70 kD. In addition, the levels of transforming grow factor-β (TGF-β) in the PFPs of patients with LSIL, HSIL and CC positively correlated with those of CD39 ( r = 0.4432 , p < 0.001 ) and CD73 ( r = 0.5786 , p < 0.001 ). These results suggest that persistent infection by HR-HPV and the concomitant production of TGF-β promote the expression of CD39 and CD73 to favor CC progression through Ado generation.

Published

2020

47. Isolation and characterization of high affinity and highly stable anti-Chikungunya virus antibodies using ALTHEA Gold Libraries™

Author

Rommel Chacón-Salinas, Rosa Camacho-Sandoval, Hugo Iván Arrieta-Oliva, Sonia Mayra Pérez-Tapia, Omar U. Guzmán-Bringas, P Contreras-Pineda, Keyla M. Gómez-Castellano, J Salinas-Trujano, J C Almagro, J Torres-Flores, Martha Pedraza-Escalona, and J C Muñoz-Herrera

Subjects

Next-Generation Sequencing, Phage display, Infectious and parasitic diseases, RC109-216, Biology, medicine.disease_cause, Antibodies, Viral, Epitope, Virus, Human Antibodies, Viral Envelope Proteins, medicine, Venezuelan equine encephalitis Virus, Humans, Chikungunya, Diagnostic, Neutralizing antibody, virus diseases, Virology, Antibodies, Neutralizing, Infectious Diseases, Capsid, Venezuelan equine encephalitis virus, biology.protein, Chikungunya Fever, Antibody, Chikungunya virus, Research Article

Abstract

Background More than 3 million infections were attributed to Chikungunya virus (CHIKV) in the 2014–2016 outbreak in Mexico, Central and South America, with over 500 deaths directly or indirectly related to this viral disease. CHIKV outbreaks are recurrent and no vaccine nor approved therapeutics exist to prevent or treat CHIKV infection. Reliable and robust diagnostic methods are thus critical to control future CHIKV outbreaks. Direct CHIKV detection in serum samples via highly specific and high affinity anti-CHIKV antibodies has shown to be an early and effective clinical diagnosis. Methods To isolate highly specific and high affinity anti-CHIKV, Chikungunya virions were isolated from serum of a patient in Veracruz, México. After purification and characterization via electron microscopy, SDS-PAGE and binding to well-characterized anti-CHIKV antibodies, UV-inactivated particles were utilized as selector in a solid-phase panning in combination with ALTHEA Gold Libraries™, as source of antibodies. The screening was based on ELISA and Next-Generation Sequencing. Results The CHIKV isolate showed the typical morphology of the virus. Protein bands in the SDS-PAGE were consistent with the size of CHIKV capsid proteins. UV-inactivated CHIKV particles bound tightly the control antibodies. The lead antibodies here obtained, on the other hand, showed high expression yield, > 95% monomeric content after a single-step Protein A purification, and importantly, had a thermal stability above 75 °C. Most of the antibodies recognized linear epitopes on E2, including the highest affinity antibody called C7. A sandwich ELISA implemented with C7 and a potent neutralizing antibody isolated elsewhere, also specific for E2 but recognizing a discontinuous epitope, showed a dynamic range of 0.2–40.0 mg/mL of UV-inactivated CHIKV purified preparation. The number of CHIKV particles estimated based on the concentration of E2 in the extract suggested that the assay could detect clinically meaningful amounts of CHIKV in serum. Conclusions The newly discovered antibodies offer valuable tools for characterization of CHIKV isolates. Therefore, the strategy here followed using whole viral particles and ALTHEA Gold Libraries™ could expedite the discovery and development of antibodies for detection and control of emergent and quickly spreading viral outbreaks.

Published

2020

48. Glycosylated Nanoparticles for Cancer-Targeted Drug Delivery

Author

Eva Ramón-Gallegos, Martha Pedraza-Escalona, Sergio Andrés Torres-Pérez, Sonia Mayra Pérez-Tapia, and Cindy Estefani Torres-Pérez

Subjects

0301 basic medicine, Cancer Research, Glycosylation, Mini Review, glycodendrimers, 02 engineering and technology, Pharmacology, lcsh:RC254-282, glycopolymers, 03 medical and health sciences, chemistry.chemical_compound, Immune system, Pharmacokinetics, Medicine, Receptor, business.industry, Cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 021001 nanoscience & nanotechnology, medicine.disease, glycoconjugates, glycosylated nanoparticles, 030104 developmental biology, Targeted drug delivery, chemistry, Oncology, Cancer cell, Drug delivery, drug delivery, cancer therapy, 0210 nano-technology, business

Abstract

Nanoparticles (NPs) are novel platforms that can carry both cancer-targeting molecules and drugs to avoid severe side effects due to nonspecific drug delivery in standard chemotherapy treatments. Cancer cells are characterized by abnormal membranes, metabolic changes, the presence of lectin receptors, glucose transporters (GLUT) overexpression, and glycosylation of immune receptors of programmed death on cell surfaces. These characteristics have led to the development of several strategies for cancer therapy, including a large number of carbohydrate-modified NPs, which have become desirable for use in cell-selective drug delivery systems because they increase nanoparticle-cell interactions and uptake of carried drugs. Currently, the potential of NP glycosylation to enhance the safety and efficacy of carried therapeutic antitumor agents has been widely acknowledged, and much information is accumulating in this field. This review seeks to highlight recent advances in NP stabilization, toxicity reduction, and pharmacokinetic improvement and the promising potential of NP glycosylation from the perspective of molecular mechanisms described for drug delivery systems for cancer therapy. From preclinical proof-of-concept to demonstration of therapeutic value in the clinic, the challenges and opportunities presented by glycosylated NPs, with a focus on their applicability in the development of nanodrugs, are discussed in this review.

Published

2020

49. Consistency of a dialyzable leucocyte extract manufactured at GMP facilities by nuclear magnetic resonance spectroscopy

Author

Sonia Mayra Pérez-Tapia, Carlos A. López-Morales, Sergio Estrada-Parra, José Enrique Herbert-Pucheta, L. Gerardo Zepeda-Vallejo, and Emilio Medina-Rivero

Subjects

Magnetic Resonance Spectroscopy, Clinical Biochemistry, Dispersity, Pharmaceutical Science, Peptide, Transfer Factor, 01 natural sciences, Analytical Chemistry, Turn (biochemistry), Consistency (statistics), Drug Discovery, Humans, Spectroscopy, chemistry.chemical_classification, Reproducibility, Chromatography, 010405 organic chemistry, Chemistry, Plant Extracts, Homogeneity (statistics), 010401 analytical chemistry, Reproducibility of Results, Nuclear magnetic resonance spectroscopy, 0104 chemical sciences, Molecular Weight, Heteronuclear molecule

Abstract

The present work describes the development and validation of a first report including several non-invasive NMR schemes to identify parameters as local chemical environments, homo- and heteronuclear site-specific spin correlations, diffusion coefficient-dependent polydispersity indexes and quantification of identified peptide entities that composes a commercial human Dialyzable Leucocyte Extract (DLE), Transferon, an oral liquid formulation of low-molecular-weight peptides. The above parameters were useful indicators to verify reproducibility, consistency and homogeneity among the DLE batches manufactured at Good Manufacturing Practice (GMP) facilities and for batch-releasing purposes in a quality control laboratory. The results showed that peptide identity of the DLE is represented with both high reproducible one-dimensional proton spectra and diffusion coefficient distributions that predicts in turn a weight-average molecular weight of around 6.7-7.4 kDa and a mean polydispersity index of 1.13. The obtained NMR peptide fingerprint of the analyzed DLE allowed to i) confirm its structural homogeneity by line-shape analysis, ii) identify and quantify its peptide content within the total solution with qNMR methods iii) to confirm the robustness of the technique as a feasible alternative for routine analysis of Natural or non-Natural Complex Drugs, such as DLEs.

Published

2020

50. Antibody-drug conjugates: the new generation of biotechnological therapies against cancer

Author

Sonia Mayra Pérez-Tapia, Emilio Medina-Rivero, Marco A. Velasco-Velázquez, and Guadalupe Melgarejo-Rubio

Subjects

Immunoconjugates, Gemtuzumab ozogamicin, medicine.drug_class, Antineoplastic Agents, Monoclonal antibody, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antigen, Antigens, Neoplasm, Neoplasms, medicine, Humans, 030212 general & internal medicine, Inotuzumab ozogamicin, biology, Cancer, General Medicine, medicine.disease, chemistry, Trastuzumab emtansine, Cancer cell, biology.protein, Cancer research, Antibody, medicine.drug, Biotechnology

Abstract

Therapeutic antibodies are recombinant proteins used in the treatment of cancer. There is a new generation of monoclonal antibodies with activity against cancer cells, known as antibody-drug conjugates. These molecules are made up of three elements: a monoclonal antibody, a highly potent cytotoxic drug, and a chemical linker that binds them together. The antibody recognizes tumor antigens, thereby allowing targeted delivery of the cytotoxic agent to cancer cells. After recognizing its antigen, the antibody-drug conjugate is endocytosed by the target cells, where the protein fraction is degraded into lysosomes, releasing the cytotoxic drug. This article reviews antibody-drug conjugates general characteristics and describes the clinical evidence of efficacy and safety of the first four approved by regulatory agencies in the United States and Europe.Los anticuerpos terapéuticos son proteínas recombinantes empleadas en el tratamiento del cáncer. Existe una nueva ­generación de anticuerpos monoclonales con actividad contra las células cancerosas, conocidos como anticuerpos conjugados a fármacos. Estas moléculas están integradas por tres elementos: un anticuerpo monoclonal, un fármaco citotóxico con alta potencia y un enlazador químico que los une. El anticuerpo reconoce antígenos tumorales, por lo que permite la entrega dirigida del agente citotóxico hacia las células cancerosas. Tras el reconocimiento de su antígeno, el anticuerpo conjugado a fármaco es endocitado por las células blanco, donde se induce la degradación lisosomal de la fracción proteica y se libera el fármaco citotóxico. En el presente artículo se revisan las características generales de los anticuerpos conjugados a fármacos y se describe la evidencia clínica de la eficacia y seguridad de los primeros cuatro aprobados por las agencias reguladoras de Estados Unidos y Europa.

Published

2020