<?xml version="1.0" encoding="UTF-8"?><?xml-stylesheet type="text/xsl" href="static/style.xsl"?><OAI-PMH xmlns="http://www.openarchives.org/OAI/2.0/" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xsi:schemaLocation="http://www.openarchives.org/OAI/2.0/ http://www.openarchives.org/OAI/2.0/OAI-PMH.xsd"><responseDate>2026-07-18T17:04:56Z</responseDate><request verb="GetRecord" identifier="oai:riubu.ubu.es:10259/7632" metadataPrefix="marc">https://riubu.ubu.es/oai/request</request><GetRecord><record><header><identifier>oai:riubu.ubu.es:10259/7632</identifier><datestamp>2023-04-01T00:05:26Z</datestamp><setSpec>com_10259_4862</setSpec><setSpec>com_10259_5086</setSpec><setSpec>com_10259_2604</setSpec><setSpec>col_10259_4863</setSpec></header><metadata><record xmlns="http://www.loc.gov/MARC21/slim" xmlns:doc="http://www.lyncode.com/xoai" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xmlns:dcterms="http://purl.org/dc/terms/" xsi:schemaLocation="http://www.loc.gov/MARC21/slim http://www.loc.gov/standards/marcxml/schema/MARC21slim.xsd">
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<subfield code="a">Simões, Rachel Siqueira de Queiroz</subfield>
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<subfield code="a">Rodríguez Lázaro, David</subfield>
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<subfield code="c">2022-02</subfield>
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<subfield code="a">Several coronaviruses (CoVs) have been identified as human pathogens, including the&#xd;
α-CoVs strains HCoV-229E and HCoV-NL63 and the β-CoVs strains HCoV-HKU1 and HCoV-OC43.&#xd;
SARS-CoV, MERS-CoV, and SARS-CoV-2 are also classified as β-coronavirus. New SARS-CoV-2 spike&#xd;
genomic variants are responsible for human-to-human and interspecies transmissibility, consequences&#xd;
of adaptations of strains from animals to humans. The receptor-binding domain (RBD) of SARS-CoV-2&#xd;
binds to receptor ACE2 in humans and animal species with high affinity, suggesting there have been&#xd;
adaptive genomic variants. New genomic variants including the incorporation, replacement, or&#xd;
deletion of the amino acids at a variety of positions in the S protein have been documented and&#xd;
are associated with the emergence of new strains adapted to different hosts. Interactions between&#xd;
mutated residues and RBD have been demonstrated by structural modelling of variants including&#xd;
D614G, B.1.1.7, B1.351, P.1, P2; other genomic variants allow escape from antibodies generated by&#xd;
vaccines. Epidemiological and molecular tools are being used for real-time tracking of pathogen&#xd;
evolution and particularly new SARS-CoV-2 variants. COVID-19 vaccines obtained from classical and&#xd;
next-generation vaccine production platforms have entered clinicals trials. Biotechnology strategies&#xd;
of the first generation (attenuated and inactivated virus–CoronaVac, CoVaxin; BBIBP-CorV), second&#xd;
generation (replicating-incompetent vector vaccines–ChAdOx-1; Ad5-nCoV; Sputnik V; JNJ-78436735&#xd;
vaccine-replicating-competent vector, protein subunits, virus-like particles–NVX-CoV2373 vaccine),&#xd;
and third generation (nucleic-acid vaccines–INO-4800 (DNA); mRNA-1273 and BNT 162b (RNA&#xd;
vaccines) have been used. Additionally, dendritic cells (LV-SMENP-DC) and artificial antigenpresenting (aAPC) cells modified with lentiviral vector have also been developed to inhibit viral&#xd;
activity. Recombinant vaccines against COVID-19 are continuously being applied, and new clinical&#xd;
trials have been tested by interchangeability studies of viral vaccines developed by classical and&#xd;
next-generation platforms.</subfield>
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<subfield code="a">http://hdl.handle.net/10259/7632</subfield>
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<datafield tag="024" ind2=" " ind1="8">
<subfield code="a">10.3390/ijerph19042392</subfield>
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<datafield tag="024" ind2=" " ind1="8">
<subfield code="a">1660-4601</subfield>
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<datafield ind1=" " ind2=" " tag="653">
<subfield code="a">Genomic variants</subfield>
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<subfield code="a">Technological platforms</subfield>
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<subfield code="a">SARS-CoV-2</subfield>
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<subfield code="a">Classical and Next-Generation Vaccine Platforms to SARS-CoV-2: Biotechnological Strategies and Genomic Variants</subfield>
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