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Review
. 2013 Apr 18;31 Suppl 2(Suppl 2):B197-203.
doi: 10.1016/j.vaccine.2012.10.074.

Desirability and feasibility of a vaccine against cytomegalovirus

Affiliations
Review

Desirability and feasibility of a vaccine against cytomegalovirus

Paul Griffiths et al. Vaccine. .

Abstract

Publication of a report from the Institute of Medicine in 2000 showing that a vaccine against cytomegalovirus (CMV) would likely be cost saving was very influential and encouraged the clinical evaluation of candidate vaccines. The major objective of a CMV vaccination program would be to reduce disease caused by congenital CMV infection, which is the leading viral cause of sensorineural hearing loss and neurodevelopmental delay. CMV has challenges as a vaccine target because it is a herpesvirus, it persists lifelong despite host immunity, infected individuals can be reinfected with new strains, overt disease occurs in those with immature or impaired immune systems and persons with this infection do not usually report symptoms. Nevertheless, natural immunity against CMV provides some protection against infection and disease, natural history studies have defined the serological and molecular biological techniques needed for endpoints in future clinical trials of vaccines and CMV is not highly communicable, suggesting that it may not be necessary to achieve very high levels of population immunity through vaccination in order to affect transmission. Three phase 2 CMV vaccine studies have been completed in the last 3 years and all report encouraging outcomes. A key international meeting was organized by the Food and Drug Administration in January 2012 at which interested parties from regulatory bodies, industry and academia discussed and prioritised designs for phase 2 and phase 3 clinical trials. Vaccines able to prevent primary infection with CMV and to boost the immune response of those already infected are desirable. The major target populations for a CMV vaccine include women of childbearing age and adolescents. Toddlers represent another potential population, since an effect of vaccine in this age group could potentially decrease transmission to adults. In addition, prospective recipients of transplants and patients with AIDS would be expected to benefit.

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Conflict of interest statement

Conflicts of interest

EM is a paid consultant in the area of CMV vaccines for Med-Immune, LLC. All other authors declare that they have no personal conflicts of interest.

Figures

Fig. 1
Fig. 1
Disease outcome per 1000 babies with congenital CMV [20]. The major long-term effects are sensorineural hearing loss (represented by a child wearing earphones):and neurodevelopmental delay.
Fig. 2
Fig. 2
Estimates of causes of deafness at birth and at 4 years in the USA [70]. GJB2 represents gap junction beta-2 gene, mtA1555G the mitochondrial A1555G mutation, and EVA, enlargement of the vestibular aqueduct.

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