Cytomegalovirus History, Biology and Treatment

Cytomegalo virus History, Biology and TreatmentHistorical Aspect piece cytomegalovirus (Hcytomegalovirus) is a very common human desoxyribonucleic acid virus. Since the startle of human life it has co-evolved with its host (McGeoch et al., 1995). Although being a part of humankind, not everybody is give (Alford et al., 1990). It was showtime isolated in 1956 by Smith where twain strains were isolated from the spitry gland and kidney of two dying infants. Cytomegalic comprehension bodies had been found in both wavers. In 1957, Weller and colleagues isolated three strains of CMV from adenoid tissues of three asymptomatic children after surgical removal. Also in 1970, they isolated three early(a) strains from liver biopsy and urine of three congenitally infected infants with CMV (Ho, 2008).In 1881, Ribbert was the first who observed the characteristic cells in the kidney of a assuageborn infant but without interpretation of these observations and that was the first description of histologic features of infection (Naraqi, 1991). The first histopathological evidenve of CMV infection was set in 1904 by Ribbert in tissues from a congenitally infected infant. Mistakenly the large inclusion-bearing cells observed at autopsy was assumed to be from protozoa. As a result, these cells were called protozoa worry cells and many workers thought that they were protozoa. After that, the similiraties between these cells and those infected by varicella-Zoster virus and herpes virus simplex virus raised the suspicion of a viral cause. In 1920, Good pasture hypothe coatd the viral cause of such inclusions (Ho, 2008).The first name proposed for CMV was salivary gland virus or salivary gland inclusion disease virus. In 1921, Good pasture and Talbot utilize the invent cytomegalia to describe the huge enlargement and alterations of infected cells. Such word was the origin of the term cytomegalovirus initially proposed by Weller and colleagues in 1960 (Weller and Hanshaw, 1 962).The procedure of the virus as an important pathogen with different clinical manifestations was significantly identified during the 1970s and 1980s. The molecular biota, immunology, and antiviral therapeutic agents had been characterized. However, establishment of preventive strategies of CMV infection and determining the role of certain genes in viral pathogenesis still need more efforts (Sung and Schleiss, 2010).Classification clement CMV, designated as HHV5, is a section of the Herpesviridae family of viruses. It is one of the 8 human herpes virusviruses (HHV) (Schleiss, 2009). The Herpesviridae family is divided into three subfamilies designated , , and . The crystallizeification into these subfamilies is ground on the features of host range, duration of reproductive cycle, cytopathology and characteristics of latent infection. DNA duration analysis, guanine and cytosine (G + C) content snd serologic reactivity of gene products be the main criteria for subdivision of e ach subfamily into genera (Hanley and Bollard, 2014). The subfamily entangles herpes simplex viruses 1 and 2 (HSV-1 and HSV-2) and varicella-zoster virus (VZV) the subfamily includes cytomegalovirus (CMV) and the roseolaviruses, human herpes viruses 6 and 7, which are responsible for the clinical syndrome of exanthem subitum (roseola infantum) in young children, and the subfamily includes Epstein-Barr virus and human herpes virus 8. All of these viruses share similarities in virion word structure and genome organization (Schleiss, 2009). Human herpesvirus classification is represented in table ( ) (Ryan and Ray, 2004).Table (1) Humah haerpesvirus (HHV) classificstionType equivalent wordSubfamilyPrimary Target CellPathophysiologySite of LatencyMeans of parcel outHHV-1Herpes simplex virus-1 (HSV-1) (Alpha)Mucoepithelial ad-lib and/or genital herpes (predominantly orofacial), as well as other herpes simplex infectionsNeuron tight-fitting contact (oral or sexually transmitted inf ection)HHV-2Herpes simplex virus-2 (HSV-2)MucoepithelialOral and/or genital herpes (predominantly genital), as well as other herpes simplex infectionsNeuronClose contact (sexually transmitted disease)HHV-3Varicella zoster virus (VZV)MucoepithelialChickenpox and shinglesNeuronRespiratory and turn up contactHHV-4Epstein-Barr virus (EBV), lymphocryptovirus (Gamma)B cells and epithelial cellsInfectious mononucleosis, Burkitt lymphoma, CNS lymphoma in AIDS patients, post-transplant lymphoproliferative syndrome (PTLD), nasopharyngeal carcinoma, HIV-associated hairy leucoplakiaB cellClose contact, transfusions, tissue transplant, and congenitalHHV-5Cytomegalovirus (CMV)(Beta)Monocyte, lymphocyte, and epithelial cellsInfectious mononucleosis-like syndrome, retinitis, etc.Monocyte, lymphocyte, and?Saliva, urine, breast milk, etcHHV-6A and 6BRoseolavirus, Herpes lymphotropic virusT cells and ?Sixth disease (roseola infantum or exanthem subitum)T cell and ?Respiratory and close contactHHV-7P ityriasis RoseaT cells and ?? (roseola infantum or exanthema subitum)T cell and ??HHV-8Kaposis sarcoma -associated herpesvirus (KSHV), a type of rhadinovirusLymphocyte, and other cellsKaposisarcoma, primary explosion lymphoma, some types of multicentric Castlemans diseaseB cellClose contact (sexual), saliva?Quoted from (Ryan and Ray , 2004).Biology of CytomegalovirusMorphologyCytomegalovirus is an windbagd virus with a double-stranded DNA genome. The three distinct regions of the CMV virus particle include an icosahedral capsid the tegument layer and an outer lipid envelope. The morphology of CMV is demonstrated in the electron microscopy (EM) studies shown in Fig. (). The capsid, which comprises 162 capsomere subunits arranged in an icosahedral symmetry, houses the viral genome, and is classically highly electron-dense when imaged by EM (Schleiss, 2011).In the virus particle, the capsid is surrounded by the tegument, a protein-rich layer containing some(prenominal) of the domin ant targets of the T-lymphocyte response to infection, including a 65-kilodalton (kDa) phosphoprotein (pp) referred to as pp65 (Kern etal., 2002). Surrounding the tegument is the envelope layer which contains several virally-encoded glycoproteins (g), including protein complexes designated as the gB complex, the gM/gN complex, and the gH/gL/gO complex. CMV-seropositive individuals gain an immune response characterized by neutralizing antibodies that target these glycoproteins (Bernstein, 2011). In accessory to luck as targets of the humoral immune response, these glycoproteins also play a central role in the binding and entry of CMV into cells (Ryckman etal., 2006). As a result of the variability in the thickness of the tegument, the complete virion varies in size from 150 to 200 nm in diameter. The genome is about 64 nm in diameter with a molecular weight of 100 x 106 to 150 x 106. The capsid is 110 nm in diameter (Subhendu et al., 2007).During the process of viral replicatio n, a variety of types of CMV particles are generated. In cell culture, CMV infection leads to the assembly and release of, in addition to infectious virions, non-infectious defective particles termed dense bodies (DB), so designated because of their characteristic highly electron-dense fashion when imaged by EM. Another type of body, designated as a noninfectious enveloped particle (NIEP), is also generated during viral replication as designated in Fig. () (Pepperl etal., 2000). The structure and protein establishment of NIEPs are comparable to those of virions, but they lack DNA and are thence not infectious (Schleiss, 2011). DBs are enveloped spherical structures that lack capsid proteins and DNA (Pepperl etal., 2000). They consist mainly of viral tegument proteins and glycoproteins. In cell culture, the biology of DBs mimics that of infectious virus, since DBs enter cells efficiently and deliver their protein components intracellularly (Mersseman etal., 2008). In principle, DB s could induce a broad range of humoral and cellular immune responses (Schleiss, 2011).Cytomegalovirus particles reveal additional levels of complexity. Using CMV gene array technology, a class of viral RNA transcripts, termed virion RNAs, has been identified in infectious virions (Bresnahan and Shenk, 2000). These RNAs, which are packaged during virion assembly, are delivered to the host cell immediately on infection, potentially allowing viral gene products to be expressed in an infected cell in front any viral transcription or host immune response occurs. The role of virion