Abstract
Herpesviruses have been isolated from a wide range of hosts including humans—for which, nine species have been designated. The human herpesviruses are highly host adapted and possess the capacity for latency, allowing them to survive in the host for life, effectively hidden from the immune system. This ability of human herpesviruses to modulate the host immune response poses particular challenges for vaccine development but at the same time proves attractive for the application of human herpesvirus vaccines to certain spheres of medicine. In this review, congenital cytomegalovirus (CMV) infection and hearing loss will be described followed by a comment on the status of current vaccine development. Secondly, the association of Epstein–Barr virus (EBV) infection with multiple sclerosis (MS) and how EBV vaccination may be of benefit will then be discussed. Prevention of congenital CMV by vaccination is an attractive proposition and several vaccines have been evaluated for potential use. Particularly challenging for the development of CMV vaccines are the needs to prevent primary infection, reinfection, and reactivation at the same time as overcoming the capacity of the virus to generate highly sophisticated immunomodulatory mechanisms. Cost and the practicalities of administering potential vaccines are also significant issues, particularly for low- and middle-income countries, where the burden of disease is greatest. An effective EBV vaccine that could prevent the 200,000 new EBV-associated malignancies which occur globally each year is not currently available. There is increasing interest in developing EBV vaccines to prevent MS and, in view of the association of infectious mononucleosis with MS, reducing childhood infectious mononucleosis is a potential intervention. Currently, there is no licensed EBV vaccine and, in order to progress the development of EBV vaccines for preventing MS, a greater understanding of the association of EBV with MS is required.
Highlights
Cytomegalovirus (CMV) and Epstein–Barr virus (EBV) are human herpesviruses belonging to the family Herpesviridae, which, as of 2018 [1], comprises 122 species grouped into 19 genera, three subfamilies and three families
This ability of human herpesviruses to modulate the host immune response [4] poses particular challenges for vaccine development [5] but at the same time proves attractive for the application of human herpesvirus vaccines to certain spheres of medicine [6,7]
Antiviral treatment of symptomatic congenital CMV central nervous system (CNS) disease is recommended; treatment options are very limited and constrained by drug toxicity, cost, and the need for evidence-based efficacy data [59]
Summary
Cytomegalovirus (CMV) and Epstein–Barr virus (EBV) are human herpesviruses belonging to the family Herpesviridae, which, as of 2018 [1], comprises 122 species grouped into 19 genera, three subfamilies and three families. The human herpesviruses are highly host adapted [2] and possess the capacity for latency [3], allowing them to survive in the host for life, effectively hidden from the immune system. The human herpesviruses are responsible for a wide range of pathologies and, currently, effective vaccination is available for only one of them, the varicella-zoster virus [8]. In this short review, the roles of CMV and EBV will be described in two diseases of neurological interest. The association of EBV infection with multiple sclerosis and how EBV vaccination may be of benefit will be discussed
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