An antigen fragment encompassing the AD2 domains of glycoprotein B from two different strains is sufficient for differentiation of primary vs. recurrent human cytomegalovirus infection by ELISA

Rothe, Markus; Pepperl-Klindworth, Sandra; Lang, Dieter; Vornhagen, Rolf; Hinderer, Walter; Weise, K.; Sonneborn, H.‐H.; Plachter, Bodo

doi:10.1002/jmv.2096

Cited by 17 publications

(11 citation statements)

References 62 publications

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“…The prevalence of reactivity to a recombinant glycoprotein B (gB AD2) fusion protein immediately after delivery was identical, encompassing about 85% of mothers in each seropositive group (T, NT) indicating recurrent maternal infection. This corresponds well to the sensitivity of this assay in seropositive blood donors (Rothe et al, 2001). Maternal virus shedding into urine or saliva was not observed in either group (T, NT).…”

Section: Hcmv Reactivation During Lactation Is a Local Processsupporting

confidence: 65%

Cytomegalovirus transmission to preterm infants during lactation

Hamprecht

Maschmann

Jahn

et al. 2008

Journal of Clinical Virology

154

114

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Section: Hcmv Reactivation During Lactation Is a Local Processsupporting

confidence: 65%

Cytomegalovirus transmission to preterm infants during lactation

Hamprecht

Maschmann

Jahn

et al. 2008

Journal of Clinical Virology

154

114

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“…ELISA using these purified recombinant proteins for the measurement of antibodies against the strain-specific gH epitopes was performed as described previously [20], with slight modification. In brief, microtiter plate wells (ELISA-PLATE 96w; Greiner Bio-One) were coated with 1 mg of purified recombinant gH-GST fusion proteins or of purified GST, and they were then blocked with 3% bovine serum albumin in phosphate buffered saline for 2 h at 37ЊC.…”

Section: Methodsmentioning

confidence: 99%

Association of the Outcome of Renal Transplantation with Antibody Response to Cytomegalovirus Strain--Specific Glycoprotein H Epitopes

Ishibashi

Tokumoto

Tanabe

et al. 2007

Clinical Infectious Diseases

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Background. Cytomegalovirus (CMV) is the most important pathogen affecting the outcome of renal transplantation. The combination of CMV-seronegative transplant recipients with CMV-seropositive transplant donors places recipients at the highest risk of CMV disease. In cases of congenital CMV infection, existing immunity only partially protected mothers from reinfection with a different genotypic strain. The effect of differences in infected CMV strains between CMV-seropositive transplant donors and CMV seropositive transplant recipients on the outcome of transplantation remains unclear.Methods. In this prospective multicenter study, the presence of antibodies against strain-specific glycoprotein H epitopes in 84 CMV-seropositive transplant donor/CMV-seropositive transplant recipient renal transplantation cases were determined, and their relationships to acute transplant rejection, CMV infection, degree of antigenemia, and CMV disease were evaluated.Results. Among the 84 donor/recipient pairs, 45 and 32 had matched and mismatched strain-specific glycoprotein H antibodies, respectively. Acute transplant rejection in the mismatched group was more frequent than it was in the matched group (63% vs. 22%;). CMV disease was also more frequently observed in the P p .005 mismatched group (28% vs. 9%;). The mismatched group had a higher level of antigenemia ( P p .026 P p ). .019Conclusions. Our results illustrate more adverse events in the cases with a CMV-seropositive transplant donor and a CMV-seropositive transplant recipient in which the glycoprotein H antibodies are mismatched, suggesting that reinfection with a different CMV strain results in more complications.

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“…These include the original design of the Chiron gB vaccine, a molecular fusion protein of 807 aa, that was mutagenized at the protease cleavage site and which contained an internal deletion of the putative membrane-spanning (TM) domain between aa 715 and 772 (48,54,55). This molecule and variant constructs of 680 (gB680) and 692 aa, from which the entire carboxyl terminus was deleted, were shown to be immunogenic in animals and humans and induced virus-neutralizing antibodies (NAb) (7,48,53,54). In fact, a plasmid expressing gB680 induced higher levels of CMV NAb than full-length gB in mice, confirming reports that it is more immunogenic than fulllength gB, making it a suitable candidate for further vaccine development (26,27).…”

mentioning

confidence: 99%

Recombinant Modified Vaccinia Virus Ankara Expressing a Soluble Form of Glycoprotein B Causes Durable Immunity and Neutralizing Antibodies against Multiple Strains of Human Cytomegalovirus

Wang

Rosa

Maas

et al. 2004

J Virol

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Human cytomegalovirus (CMV) is a viral pathogen that infects both genders, who remain asymptomatic unless they receive immunosuppressive drugs or acquire infections that cause reactivation of latent virus. CMV infection also causes serious birth defects following primary maternal infection during gestation. A safe and effective vaccine to limit disease in this population continues to be elusive. A well-studied antigen is glycoprotein B (gB), which is the principal target of neutralizing antibodies (NAb) towards CMV in humans and has been implicated as the viral partner in the receptor-mediated infection by CMV in a variety of cell types. Antibody-mediated virus neutralization has been proposed as a mechanism by which host immunity could modify primary infection. Towards this goal, an attenuated poxvirus, modified vaccinia virus Ankara (MVA), has been constructed to express soluble CMV gB (gB680-MVA) to induce CMV NAb. Very high levels of gB-specific CMV NAb were produced after two doses of the viral vaccine. NAb were durable within a twofold range for up to 6 months. Neutralization titers developed in immunized mice are equivalent to titers found clinically after natural infection. This viral vaccine, expressing gB derived from CMV strain AD169, induced antibodies that neutralized CMV strains of three different genotypes. Remarkably, preexisting MVA and vaccinia virus (poxvirus) immunity did not interfere with subsequent immunizations of gB680-MVA. The safety characteristics of MVA, combined with the robust immune response to CMV gB, suggest that this approach could be rapidly translated into the clinic.Human cytomegalovirus (HCMV) is a member of the herpesvirus family. It is a major cause of congenital disease, resulting in an estimated 4,000 cases of symptomatic congenital cytomegalovirus (CMV) infection per year in the United States (58). An effective CMV vaccine that can prevent or reduce CMV-associated disease is highly desirable. Early studies have indicated that HCMV gB is the major target of NAb that are induced by naturally acquired CMV infection (16,39). It is the most highly conserved envelope glycoprotein of human herpesviruses (38). Thus, CMV gB has been an attractive candidate for CMV vaccine development. CMV gB vaccines using recombinant gB protein expressed from plasmid DNA and gB expressed in several different viral vectors (ALVAC, adenovirus, and vaccinia virus [VV]) have been investigated with animal models (9,13,23,26,31,40,54). Safety and moderate immunogenicity have been demonstrated with these vaccines, but no licensed CMV vaccine is available. A live attenuated Towne strain of CMV, either alone or with a gB subunit vaccine as a prime-boost, have also been evaluated in human subjects (1, 2, 48).Full-length CMV gB is synthesized as a 907-amino acid (aa) precursor in CMV-infected cells with a predicted molecular mass of 105 kDa, but it can be glycosylated to form a 170-kDa modified protein (17). To enable pharmaceutical development, truncated and secretable forms of gB were derived. These in...

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An antigen fragment encompassing the AD2 domains of glycoprotein B from two different strains is sufficient for differentiation of primary vs. recurrent human cytomegalovirus infection by ELISA

Cited by 17 publications

References 62 publications

Cytomegalovirus transmission to preterm infants during lactation

Cytomegalovirus transmission to preterm infants during lactation

Association of the Outcome of Renal Transplantation with Antibody Response to Cytomegalovirus Strain--Specific Glycoprotein H Epitopes

Recombinant Modified Vaccinia Virus Ankara Expressing a Soluble Form of Glycoprotein B Causes Durable Immunity and Neutralizing Antibodies against Multiple Strains of Human Cytomegalovirus

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