Your search keyword '"Alexis J. Romero-Díaz"' showing total 6 results

1. Characterization and comparability of biosimilars: A filgrastim case of study and regulatory perspectives for Latin America

Author

Karina Mendoza-Macedo, Alexis J. Romero-Díaz, Mariana P. Miranda-Hernández, Víctor R. Campos-García, Nancy D. Ramírez-Ibañez, L. Carmina Juárez-Bayardo, Karen Moreno-Duran, Miriam S. Cedillo-Robles, Nestor O. Pérez, Helgi Jung-Cook, Luis F. Flores-Ortiz, and Emilio Medina-Rivero

Subjects

Bio therapeutic, Comparability, Critical quality attributes, Developing countries, Generics, Health policies, High quality biosimilars, Regulation, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5

Abstract

Background: Developing countries have an estimate of ten times more approved biosimilars than developed countries. This disparity demands the need of an objective regulation that incorporates health policies according to the technological and economical capabilities of each country. One of the challenges lies on the establishment of comparability principles based on a physicochemical and biological characterization that should determine the extent of additional non-clinical and clinical studies. This is particularly relevant for licensed biosimilars in developing countries, which have an extensive clinical experience since their approval as generics, in some cases more than a decade. To exemplify the current status of biosimilars in Mexico, a characterization exercise was conducted on licensed filgrastim biosimilars using pharmacopeial and extended characterization methodologies. Results: Most of the evaluated products complied with the pharmacopeial criteria and showed comparability in their Critical Quality Attributes (CQAs) towards the reference product. These results were expected in accordance with their equivalent performance during their licensing as generics. Accordingly, a rational approval and registration renewal scheme for biosimilars is proposed, that considers the proper identification of CQAs and its thoroughly evaluation using selected techniques. Conclusions: This approach provides support to diminish uncertainty of exhibiting different pharmacological profiles and narrows or even avoids the necessity of comparative clinical studies. Ultimately, this proposal is intended to improve the accessibility to high quality biosimilars in Latin America and other developing countries.

Published

2016

2. Comparability of a Three-Dimensional Structure in Biopharmaceuticals Using Spectroscopic Methods

Author

Víctor Pérez Medina Martínez, Mario E. Abad-Javier, Alexis J. Romero-Díaz, Francisco Villaseñor-Ortega, Néstor O. Pérez, Luis F. Flores-Ortiz, and Emilio Medina-Rivero

Subjects

Analytical chemistry, QD71-142

Abstract

Protein structure depends on weak interactions and covalent bonds, like disulfide bridges, established according to the environmental conditions. Here, we present the validation of two spectroscopic methodologies for the measurement of free and unoxidized thiols, as an attribute of structural integrity, using 5,5′-dithionitrobenzoic acid (DTNB) and DyLight Maleimide (DLM) as derivatizing agents. These methods were used to compare Rituximab and Etanercept products from different manufacturers. Physicochemical comparability was demonstrated for Rituximab products as DTNB showed no statistical differences under native, denaturing, and denaturing-reducing conditions, with Student’s t-test P values of 0.6233, 0.4022, and 0.1475, respectively. While for Etanercept products no statistical differences were observed under native (P=0.0758) and denaturing conditions (P=0.2450), denaturing-reducing conditions revealed cysteine contents of 98% and 101%, towards the theoretical value of 58, for the evaluated products from different Etanercept manufacturers. DLM supported equality between Rituximab products under native (P=0.7499) and denaturing conditions (P=0.8027), but showed statistical differences among Etanercept products under native conditions (P

Published

2014

3. Optimization of a recombinant human growth hormone purification process using quality by design

Author

Carolina Ortiz-Enriquez, Hugo F Cueto-Rojas, Emilio Medina-Rivero, Mariana P. Miranda-Hernández, Luis F. Flores-Ortiz, Alexis J. Romero-Díaz, Néstor O. Pérez, Carlos A. López-Morales, Ana V. Hernández-Moreno, Norberto Cruz-García, and Rodolfo Salazar-Ceballos

Subjects

0301 basic medicine, Computer science, 01 natural sciences, Biochemistry, Quality by Design, 03 medical and health sciences, Capillary electrophoresis, Humans, Process optimization, Process engineering, Active ingredient, Chromatography, Reverse-Phase, Downstream processing, business.industry, Human growth hormone, 010401 analytical chemistry, Electrophoresis, Capillary, General Medicine, Recombinant Proteins, 0104 chemical sciences, 030104 developmental biology, Solubility, Growth Hormone, Scientific method, Chromatography, Gel, business, Critical quality attributes, Biotechnology

Abstract

This work describes a strategy to optimize a downstream processing of a recombinant human growth hormone (rhGH) by incorporating a quality by design approach toward meeting higher quality specifications. The optimized process minimized the presence of impurities and degradation by-products during manufacturing by the establishment of in-process controls. Capillary zone electrophoresis, reverse phase, and size-exclusion chromatographies were used as analytical techniques to establish new critical process parameters for the solubilization, capture, and intermediate purification steps aiming to maintain rhGH quality by complying with pharmacopeial specifications. The results indicated that the implemented improvements in the process allowed the optimization of the specific recovery and purification of rhGH without compromising its quality. In addition, this optimization facilitated the stringent removal of the remaining impurities in further polishing stages, as demonstrated by the analysis of the obtained active pharmaceutical ingredient.

Published

2016

4. Characterization and comparability of biosimilars: A filgrastim case of study and regulatory perspectives for Latin America

Author

Helgi Jung-Cook, Karina Mendoza-Macedo, Nancy D. Ramírez-Ibanez, Mariana P. Miranda-Hernández, Víctor R. Campos-García, Karen Moreno-Duran, Alexis J. Romero-Díaz, L. Carmina Juárez-Bayardo, Néstor O. Pérez, Miriam S. Cedillo-Robles, Luis F. Flores-Ortiz, and Emilio Medina-Rivero

Subjects

0301 basic medicine, media_common.quotation_subject, lcsh:Biotechnology, Developing country, 01 natural sciences, Applied Microbiology and Biotechnology, Developing countries, Health policies, 03 medical and health sciences, Serif, lcsh:TP248.13-248.65, Comparability, Generics, Critical quality attributes, Quality (business), lcsh:QH301-705.5, media_common, 010401 analytical chemistry, Biosimilar, 0104 chemical sciences, Identification (information), 030104 developmental biology, Risk analysis (engineering), lcsh:Biology (General), High quality biosimilars, Bio therapeutic, Business, Developed country, Biotechnology, Regulation

Abstract

Background: Developing countries have an estimate of ten times more approved biosimilars than developed countries. This disparity demands the need of an objective regulation that incorporates health policies according to the technological and economical capabilities of each country. One of the challenges lies on the establishment of comparability principles based on a physicochemical and biological characterization that should determine the extent of additional non-clinical and clinical studies. This is particularly relevant for licensed biosimilars in developing countries, which have an extensive clinical experience since their approval as generics, in some cases more than a decade. To exemplify the current status of biosimilars in Mexico, a characterization exercise was conducted on licensed filgrastim biosimilars using pharmacopeial and extended characterization methodologies. Results: Most of the evaluated products complied with the pharmacopeial criteria and showed comparability in their Critical Quality Attributes (CQAs) towards the reference product. These results were expected in accordance with their equivalent performance during their licensing as generics. Accordingly, a rational approval and registration renewal scheme for biosimilars is proposed, that considers the proper identification of CQAs and its thoroughly evaluation using selected techniques. Conclusions: This approach provides support to diminish uncertainty of exhibiting different pharmacological profiles and narrows or even avoids the necessity of comparative clinical studies. Ultimately, this proposal is intended to improve the accessibility to high quality biosimilars in Latin America and other developing countries. Normal 0 21 false false false ES-MX JA X-NONE /* Style Definitions */ table.MsoNormalTable {mso-style-name:"Tabla normal"; mso-tstyle-rowband-size:0; mso-tstyle-colband-size:0; mso-style-noshow:yes; mso-style-priority:99; mso-style-parent:""; mso-padding-alt:0cm 5.4pt 0cm 5.4pt; mso-para-margin:0cm; mso-para-margin-bottom:.0001pt; mso-pagination:widow-orphan; font-size:10.0pt; font-family:"Cambria","serif"; mso-ansi-language:ES-MX;}

Published

2016

5. Physicochemical and Biological Characterization of a Biosimilar Trastuzumab

Author

Víctor R. Campos-García, Alexis J. Romero-Díaz, Luis F. Flores-Ortiz, Mariana P. Miranda-Hernández, Carlos A. López-Morales, Nancy D. Ramírez-Ibanez, Emilio Medina-Rivero, L. Carmina Juárez-Bayardo, Néstor O. Pérez, and Nelly Piña-Lara

Subjects

Article Subject, lcsh:Medicine, Antineoplastic Agents, Computational biology, Pharmacology, General Biochemistry, Genetics and Molecular Biology, World health, Biosimilar Pharmaceuticals, Trastuzumab, Cell Line, Tumor, medicine, Humans, Degree of similarity, Potential impact, General Immunology and Microbiology, business.industry, lcsh:R, Biosimilar, General Medicine, Reference product, Pharmacodynamics, Drug Screening Assays, Antitumor, business, Research Article, medicine.drug

Abstract

According to the World Health Organization, the incidence of malignant neoplasms and endocrine, blood, and immune disorders will increase in the upcoming decades along with the demand of affordable treatments. In response to this need, the development of biosimilar drugs is increasing worldwide. The approval of biosimilars relies on the compliance with international guidelines, starting with the demonstration of similarity in their physicochemical and functional properties against the reference product. Subsequent clinical studies are performed to demonstrate similar pharmacological behavior and to diminish the uncertainty related to their safety and efficacy. Herein we present a comparability exercise between a biosimilar trastuzumab and its reference product, by using a hierarchical strategy with an orthogonal approach, to assess the physicochemical and biological attributes with potential impact on its pharmacokinetics, pharmacodynamics, and immunogenicity. Our results showed that the high degree of similarity in the physicochemical attributes of the biosimilar trastuzumab with respect to the reference product resulted in comparable biological activity, demonstrating that a controlled process is able to provide consistently the expected product. These results also constitute the basis for the design of subsequent delimited pharmacological studies, as they diminish the uncertainty of exhibiting different profiles.

Published

2015

6. Comparability of a Three-Dimensional Structure in Biopharmaceuticals Using Spectroscopic Methods

Author

Luis F. Flores-Ortiz, Mario E. Abad-Javier, Francisco Villaseñor-Ortega, Néstor O. Pérez, Emilio Medina-Rivero, Alexis J. Romero-Díaz, and Víctor Pérez Medina Martínez

Subjects

chemistry.chemical_classification, Circular dichroism, Chromatography, lcsh:QD71-142, Article Subject, DTNB, General Chemical Engineering, Dithionitrobenzoic Acid, lcsh:Analytical chemistry, Bioinformatics, Computer Science Applications, Analytical Chemistry, chemistry.chemical_compound, Protein structure, chemistry, Covalent bond, Thiol, Instrumentation, Maleimide, Cysteine, Research Article

Abstract

Protein structure depends on weak interactions and covalent bonds, like disulfide bridges, established according to the environmental conditions. Here, we present the validation of two spectroscopic methodologies for the measurement of free and unoxidized thiols, as an attribute of structural integrity, using 5,5′-dithionitrobenzoic acid (DTNB) and DyLight Maleimide (DLM) as derivatizing agents. These methods were used to compare Rituximab and Etanercept products from different manufacturers. Physicochemical comparability was demonstrated for Rituximab products as DTNB showed no statistical differences under native, denaturing, and denaturing-reducing conditions, with Student’st-testPvalues of 0.6233, 0.4022, and 0.1475, respectively. While for Etanercept products no statistical differences were observed under native (P=0.0758) and denaturing conditions (P=0.2450), denaturing-reducing conditions revealed cysteine contents of 98% and 101%, towards the theoretical value of 58, for the evaluated products from different Etanercept manufacturers. DLM supported equality between Rituximab products under native (P=0.7499) and denaturing conditions (P=0.8027), but showed statistical differences among Etanercept products under native conditions (P<0.001). DLM suggested that Infinitam has fewer exposed thiols than Enbrel, although DTNB method, circular dichroism (CD), fluorescence (TCSPC), and activity (TNFαneutralization) showed no differences. Overall, this data revealed the capabilities and drawbacks of each thiol quantification technique and their correlation with protein structure.

Published

2014