Detection of glycoproteins B and H genotypes to predict the development of Cytomegalovirus disease in solid organ transplant recipients
•Mixed gB genotypes are associated with clinical manifestations and higher viral loads.•gB3 and gH1 genotypes are detected in patients who present with asymptomatic viremia.•The detection of gB and gH genotypes can help to predict CMV disease development. Our study focuses on the role that human Cyt...
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Published in | Journal of clinical virology Vol. 109; pp. 50 - 56 |
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Language | English |
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01.12.2018
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Abstract | •Mixed gB genotypes are associated with clinical manifestations and higher viral loads.•gB3 and gH1 genotypes are detected in patients who present with asymptomatic viremia.•The detection of gB and gH genotypes can help to predict CMV disease development.
Our study focuses on the role that human Cytomegalovirus (CMV) genotypes play in the development of disease.
(1) To analyze the frequency of various genotype envelope proteins (gB, gH) in a group of solid organ transplant (SOT) recipients; (2) to assess their correlation with CMV disease; (3) to study the association between any of the genotypes and viral loads.
A retrospective observational study conducted by analyzing CMV gB and gH genotypes detected with real-time polymerase chain reaction (PCR)-specific assays in 162 CMV-positive blood samples from 62 SOT recipients. Demographic, clinical, and microbiological data were recorded.
Mixed gB genotypes were associated with viral syndrome (70%, p = .004), earlier presentation of symptoms (48.27 ± 27.03 versus 74.33 ± 47.25 days, respectively, p = .001), and higher median of the plasma viral load log10 (UI/ml) than infection with a single genotype (p = .004). Furthermore, the gB3 genotype was detected more frequently in patients who presented with asymptomatic viremia (77.27%, p < .0001).
The gH1 genotype was more frequent (65%) in patients who presented with asymptomatic viremia (p = .003), and it caused infection later than gH2 or the mixed genotype (84.88 ± 48.10 versus 57.91 ± 39.18 days, respectively, p < .001).
Patients who presented mixed gB genotypes more frequently developed clinical manifestations and earlier, higher, plasma viral loads. The detection of gB and gH genotypes by real-time PCR can provide relevant information to stratify the risk of SOT recipients to develop symptomatic infection by CMV. |
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AbstractList | BACKGROUNDOur study focuses on the role that human Cytomegalovirus (CMV) genotypes play in the development of disease. OBJECTIVES(1) To analyze the frequency of various genotype envelope proteins (gB, gH) in a group of solid organ transplant (SOT) recipients; (2) to assess their correlation with CMV disease; (3) to study the association between any of the genotypes and viral loads. STUDY DESIGNA retrospective observational study conducted by analyzing CMV gB and gH genotypes detected with real-time polymerase chain reaction (PCR)-specific assays in 162 CMV-positive blood samples from 62 SOT recipients. Demographic, clinical, and microbiological data were recorded. RESULTSMixed gB genotypes were associated with viral syndrome (70%, p = .004), earlier presentation of symptoms (48.27 ± 27.03 versus 74.33 ± 47.25 days, respectively, p = .001), and higher median of the plasma viral load log10 (UI/ml) than infection with a single genotype (p = .004). Furthermore, the gB3 genotype was detected more frequently in patients who presented with asymptomatic viremia (77.27%, p < .0001). The gH1 genotype was more frequent (65%) in patients who presented with asymptomatic viremia (p = .003), and it caused infection later than gH2 or the mixed genotype (84.88 ± 48.10 versus 57.91 ± 39.18 days, respectively, p < .001). CONCLUSIONSPatients who presented mixed gB genotypes more frequently developed clinical manifestations and earlier, higher, plasma viral loads. The detection of gB and gH genotypes by real-time PCR can provide relevant information to stratify the risk of SOT recipients to develop symptomatic infection by CMV. Our study focuses on the role that human Cytomegalovirus (CMV) genotypes play in the development of disease. (1) To analyze the frequency of various genotype envelope proteins (gB, gH) in a group of solid organ transplant (SOT) recipients; (2) to assess their correlation with CMV disease; (3) to study the association between any of the genotypes and viral loads. A retrospective observational study conducted by analyzing CMV gB and gH genotypes detected with real-time polymerase chain reaction (PCR)-specific assays in 162 CMV-positive blood samples from 62 SOT recipients. Demographic, clinical, and microbiological data were recorded. Mixed gB genotypes were associated with viral syndrome (70%, p = .004), earlier presentation of symptoms (48.27 ± 27.03 versus 74.33 ± 47.25 days, respectively, p = .001), and higher median of the plasma viral load log (UI/ml) than infection with a single genotype (p = .004). Furthermore, the gB3 genotype was detected more frequently in patients who presented with asymptomatic viremia (77.27%, p < .0001). The gH1 genotype was more frequent (65%) in patients who presented with asymptomatic viremia (p = .003), and it caused infection later than gH2 or the mixed genotype (84.88 ± 48.10 versus 57.91 ± 39.18 days, respectively, p < .001). Patients who presented mixed gB genotypes more frequently developed clinical manifestations and earlier, higher, plasma viral loads. The detection of gB and gH genotypes by real-time PCR can provide relevant information to stratify the risk of SOT recipients to develop symptomatic infection by CMV. •Mixed gB genotypes are associated with clinical manifestations and higher viral loads.•gB3 and gH1 genotypes are detected in patients who present with asymptomatic viremia.•The detection of gB and gH genotypes can help to predict CMV disease development. Our study focuses on the role that human Cytomegalovirus (CMV) genotypes play in the development of disease. (1) To analyze the frequency of various genotype envelope proteins (gB, gH) in a group of solid organ transplant (SOT) recipients; (2) to assess their correlation with CMV disease; (3) to study the association between any of the genotypes and viral loads. A retrospective observational study conducted by analyzing CMV gB and gH genotypes detected with real-time polymerase chain reaction (PCR)-specific assays in 162 CMV-positive blood samples from 62 SOT recipients. Demographic, clinical, and microbiological data were recorded. Mixed gB genotypes were associated with viral syndrome (70%, p = .004), earlier presentation of symptoms (48.27 ± 27.03 versus 74.33 ± 47.25 days, respectively, p = .001), and higher median of the plasma viral load log10 (UI/ml) than infection with a single genotype (p = .004). Furthermore, the gB3 genotype was detected more frequently in patients who presented with asymptomatic viremia (77.27%, p < .0001). The gH1 genotype was more frequent (65%) in patients who presented with asymptomatic viremia (p = .003), and it caused infection later than gH2 or the mixed genotype (84.88 ± 48.10 versus 57.91 ± 39.18 days, respectively, p < .001). Patients who presented mixed gB genotypes more frequently developed clinical manifestations and earlier, higher, plasma viral loads. The detection of gB and gH genotypes by real-time PCR can provide relevant information to stratify the risk of SOT recipients to develop symptomatic infection by CMV. |
Author | Folgueira, Lola Prieto, Columbiana Hernando, Susana Barrado, Laura |
Author_xml | – sequence: 1 givenname: Laura orcidid: 0000-0002-2578-2593 surname: Barrado fullname: Barrado, Laura email: laurajesus.barrado@salud.madrid.org organization: Virology Laboratory, Clinical Microbiology Department, University Hospital 12 de Octubre, Avda. de Córdoba s/n, 28041 Madrid, Spain – sequence: 2 givenname: Columbiana surname: Prieto fullname: Prieto, Columbiana organization: Virology Laboratory, Clinical Microbiology Department, University Hospital 12 de Octubre, Avda. de Córdoba s/n, 28041 Madrid, Spain – sequence: 3 givenname: Susana surname: Hernando fullname: Hernando, Susana organization: Virology Laboratory, Clinical Microbiology Department, University Hospital 12 de Octubre, Avda. de Córdoba s/n, 28041 Madrid, Spain – sequence: 4 givenname: Lola surname: Folgueira fullname: Folgueira, Lola organization: Virology Laboratory, Clinical Microbiology Department, University Hospital 12 de Octubre, Avda. de Córdoba s/n, 28041 Madrid, Spain |
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CitedBy_id | crossref_primary_10_3390_v13061106 crossref_primary_10_1016_j_diagmicrobio_2020_115075 crossref_primary_10_1111_tid_13615 crossref_primary_10_1007_s40121_021_00457_z crossref_primary_10_1055_s_0040_1713001 crossref_primary_10_3390_v13071370 crossref_primary_10_1080_15513815_2020_1765916 crossref_primary_10_3390_ph17040428 |
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Keywords | Transplantation Prognosis CMV genotypes Viral load |
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Snippet | •Mixed gB genotypes are associated with clinical manifestations and higher viral loads.•gB3 and gH1 genotypes are detected in patients who present with... Our study focuses on the role that human Cytomegalovirus (CMV) genotypes play in the development of disease. (1) To analyze the frequency of various genotype... BACKGROUNDOur study focuses on the role that human Cytomegalovirus (CMV) genotypes play in the development of disease. OBJECTIVES(1) To analyze the frequency... |
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SubjectTerms | CMV genotypes Prognosis Transplantation Viral load |
Title | Detection of glycoproteins B and H genotypes to predict the development of Cytomegalovirus disease in solid organ transplant recipients |
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