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Human betaherpesvirus 5

November 27, 2023

"HCMV" redirects here. For the airport with the same ICAO code, see Burao Airport.

Human betaherpesvirus 5, also called human cytomegalovirus (HCMV),[2] is species of virus in the genus Cytomegalovirus, which in turn is a member of the viral family known as Herpesviridae or herpesviruses. It is also commonly called CMV.[3] Within Herpesviridae, HCMV belongs to the Betaherpesvirinae subfamily, which also includes cytomegaloviruses from other mammals.[4] CMV is a double-stranded DNA virus.[5]

Human cytomegalovirus
SpecialtyInfectious disease
CausesHuman betaherpesvirus 5
Human betaherpesvirus 5
CMV infection of a human lung pneumocyte
Virus classification
(unranked): Virus
Realm: Duplodnaviria
Kingdom: Heunggongvirae
Phylum: Peploviricota
Class: Herviviricetes
Order: Herpesvirales
Family: Orthoherpesviridae
Genus: Cytomegalovirus
Species:
Human betaherpesvirus 5
Synonyms[1]
  • Human herpesvirus 5

Although they may be found throughout the body, HCMV infections are frequently associated with the salivary glands.[4] HCMV infection is typically unnoticed in healthy people, but can be life-threatening for the immunocompromised, such as HIV-infected persons, organ transplant recipients, or newborn infants.[3] Congenital cytomegalovirus infection can lead to significant morbidity and even death. After infection, HCMV remains latent within the body throughout life and can be reactivated at any time. Eventually, it may cause mucoepidermoid carcinoma and possibly other malignancies[6] such as prostate cancer[7] and breast cancer.[8]

HCMV is found in all geographic locations and all socioeconomic groups, and infects between 60% and 70% of adults in the first world and almost 100% in the third world.[9] Of all herpes viruses, HCMV harbors the most genes dedicated to altering (evading) innate and adaptive host immunity and represents a lifelong burden of antigenic T cell surveillance and immune dysfunction.[10] Commonly it is indicated by the presence of antibodies in the general population.[3] Seroprevalence is age-dependent: 58.9% of individuals aged 6 and older are infected with CMV while 90.8% of individuals aged 80 and older are positive for HCMV.[11] HCMV is also the virus most frequently transmitted to a developing fetus.[12] HCMV infection is more widespread in developing countries and in communities with lower socioeconomic status and represents the most significant viral cause of birth defects in industrialized countries. Congenital HCMV is the leading infectious cause of deafness, learning disabilities, and intellectual disability in children.[13] CMV also "seems to have a large impact on immune parameters in later life and may contribute to increased morbidity and eventual mortality."[14]

Signs and symptoms edit

Human betaherpesvirus 5 infection has a classic triad of symptoms: fever, peaking in the late afternoon or early evening; pharyngitis, usually exudative; and symmetrical adenopathy.[15][16][17]

Virology edit

Transmission edit

The mode of HCMV transmission from person to person is unknown, but is presumed to occur through bodily fluids, including saliva, urine, blood, and tears.[18] Cytomegalovirus is most commonly transmitted through kissing and sexual intercourse. It can also be transferred from an infected mother to her unborn child.[4] Infection requires close, intimate contact with a person secreting the virus in their saliva, urine, or other bodily fluids. CMV can be transmitted sexually and via breast milk, and also occurs through receiving transplanted organs or blood transfusions.[19] Although HCMV is not highly contagious, it has been shown to spread in households and among young children in day care centers.[3]

Replication edit

HCMV replicates within infected endothelial cells[20] at a slow rate, taking about five days in cell culture.[21] It also infects fibroblasts, which requires expression of only a trimeric viral receptor complex, rather than the full pentameric complex that is required for infection of endothelial and epithelial cells.[22] Like other herpesviruses, HCMV expresses genes in a temporally controlled manner.[23][24] Immediate early genes (0–4 hours after infection) are involved in the regulation of transcription, followed by early genes (4–48 hours after infection) which are involved in viral DNA replication and further transcriptional regulation.[23] Late genes are expressed during the remainder of infection up to viral egress and typically code for structural proteins. While HCMV encodes for its own functional DNA polymerase, the virus makes use of the host RNA polymerase for the transcription of all of its genes.[25]

In disseminated cytomegalovirus infections, as may be seen in the context of an immunosuppressed host, the virus is readily transmitted between polymorphonuclear leukocytes (PM-NLs) and endothelial cells. Infected endothelial cells produce cytokines that attract PM-NLs, which then adhere to the endothelium by interactions between their CD18-containing cell surface integrins and the endothelial-expressed ICAM-1. Microfusions between the cells then take place in a manner dependent on expression of the viral gene locus UL128L.[22]

Synthesis of the viral double-stranded DNA genome occurs at the host cell nucleus within specialized viral replication compartments.[26]

Nearly 75% of the genes encoded by HCMV strain AD169 can be deleted and still result in the production of infectious virus.[27] This suggests that the virus focuses on avoiding the host immune system for a timely entrance into latency.[28]

At-risk populations edit

CMV infections are most significant in the perinatal period and in people who are immunocompromised.

Pregnancy and congenital infection edit

Main article: Congenital cytomegalovirus infection

HCMV is one of the vertically transmitted infections that lead to congenital abnormalities. (Others are: Toxoplasmosis, Rubella, and Herpes simplex.) Congenital HCMV infection occurs when the mother has a primary infection during pregnancy.[29][30][31]

Up to 5 of every 1,000 live births are infected. Five percent develop multiple handicaps, and develop cytomegalic inclusion disease with nonspecific signs that resemble rubella. Another five percent later develop cerebral calcification (decreasing IQ levels dramatically and causing sensorineural deafness and psychomotor retardation).[citation needed]

However, infants born preterm and infected with HCMV after birth may experience cognitive and motor impairments later in life.[32]

Immunocompromised adults edit

CMV infection or reactivation in people whose immune systems are compromised—for example people who have received transplants or are significantly burned—causes illness and increases the risk of death.[33][34]

CMV reactivation is commonly seen in people with severe colitis.[35]

Specific disease entities recognized in those people are

People without CMV infection who are given organ transplants from CMV-infected donors require prophylactic treatment with valganciclovir (ideally) or ganciclovir, and regular serological monitoring to detect a rising CMV titre; if treated early establishment of a potentially life-threatening infection can be prevented.[37]

Immunocompetent adults edit

CMV infections can still be of clinical significance in adult immunocompetent populations.[38]

The question of whether latent CMV infection has any negative effects on people who are otherwise healthy has been debated; as of 2016 the answer was not clear, but discussions had focused on whether latent CMV might increase the risk of some cardiovascular diseases and cancers.[33]

Pathogenesis edit

 

Most healthy people who are infected by HCMV after birth have no symptoms.[3] Some develop a syndrome similar to infectious mononucleosis or glandular fever,[43] with prolonged fever, and a mild hepatitis. A sore throat is common. After infection, the virus remains latent in lymphocytes in the body for the rest of the person's life. Overt disease rarely occurs unless immunity is suppressed either by drugs, infection or old age. Initial HCMV infection, which often is asymptomatic, is followed by a prolonged, inapparent infection during which the virus resides in mononuclear cells without causing detectable damage or clinical illness.[44]

Infectious CMV may be shed in the bodily fluids of any infected person, and can be found in urine, saliva, blood, tears, semen, and breast milk. The shedding of virus can occur intermittently, without any detectable signs or symptoms.

 
Micrograph of CMV placentitis. One cell on the image (centre) has the characteristic large nucleus with peri-nuclear clearing. Two cells (centre-right) have the characteristic (cytoplasmic) viral inclusion bodies (small pink globules). H&E stain.

CMV infection can be demonstrated microscopically by the detection of intranuclear inclusion bodies. On H&E staining, the inclusion bodies stain dark pink and are called "owl's eye" inclusion bodies.[45]

HCMV infection is important to certain high-risk groups.[46] Major areas of risk of infection include pre-natal or postnatal infants and immunocompromised individuals, such as organ transplant recipients, persons with leukemia, or those infected with human immunodeficiency virus (HIV). In HIV infected persons, HCMV is considered an AIDS-defining infection, indicating that the T-cell count has dropped to low levels.

Lytically replicating viruses disrupt the cytoskeleton, causing massive cell enlargement, which is the source of the virus' name.

A study published in 2009 links infection with CMV to high blood pressure in mice, and suggests that the result of CMV infection of blood vessel endothelium in humans is a major cause of atherosclerosis.[47] Researchers also found that when the cells were infected with CMV, they created renin, a protein known to contribute to high blood pressure.

Human CMV causes cellular senescence, which could contribute to chronic inflammation (inflammaging).[48] Human CMV is also linked to age-associated T cell dysfunction, contributing to immunosenescence.[48] COVID-19 symptom severity is associated with CMV, although the exact mechanism has not been elucidated.[49]

CMV encodes a protein, UL16, which is involved in the immune evasion of NK cell responses. It binds to ligands ULBP1, ULBP2 and MICB of NK cell activating receptor NKG2D, which prevents their surface expression. These ligands are normally upregulated in times of cellular stress, such as in viral infection, and by preventing their upregulation, CMV can prevent its host cell from dying due to NK cells[50]

A substantial portion of the immune system is involved in continuously controlling CMV, which drains the resources of the immune system.[51][52] Death rates from infectious disease accelerate with age,[53] and CMV infection correlates with reduced effectiveness of vaccination.[54] Persons with the highest levels of CMV antibodies have a much higher risk of death from all causes compared with persons having few or no antibodies.[55][56]

Diagnosis edit

 
Micrograph of CMV placentitis.

Most infections with CMV go undiagnosed, as the virus usually produces few, if any, symptoms and tends to reactivate intermittently without symptoms. Persons who have been infected with CMV develop antibodies to the virus, which persist in the body for the lifetime of that individual. A number of laboratory tests that detect these antibodies to CMV have been developed to determine if infection has occurred and are widely available from commercial laboratories. In addition, the virus can be cultured from specimens obtained from urine, throat swabs, bronchial lavages and tissue samples to detect active infection. Both qualitative and quantitative polymerase chain reaction (PCR) testing for CMV are available as well, allowing physicians to monitor the viral load of people infected with CMV.

The CMV pp65 antigenemia test is an immunofluorescence-based assay which utilizes an indirect immunofluorescence technique for identifying the pp65 protein of cytomegalovirus in peripheral blood leukocytes.[57] The CMV pp65 assay is widely used for monitoring CMV infection and its response to antiviral treatment in people who are under immunosuppressive therapy and have had renal transplantation surgery, as the antigenemia results are obtained about 5 days before the onset of symptomatic CMV disease. The advantage of this assay is the rapidity in providing results in a few hours and that the pp65 antigen determination represents a useful criterion for the physician to initiate antiviral therapy. The major disadvantage of the pp65 assay is that only a limited number of samples can be processed per test batch.

CMV should be suspected if a person has symptoms of infectious mononucleosis but has negative test results for mononucleosis and Epstein–Barr virus, or if they show signs of hepatitis, but have negative test results for hepatitis A, B, and C.

For best diagnostic results, laboratory tests for CMV antibody should be performed by using paired serum samples. One blood sample should be taken upon suspicion of CMV, and another one taken within 2 weeks. A virus culture can be performed any time the person is symptomatic. Laboratory testing for antibodies to CMV can be performed to determine if a woman has already had CMV infection. However, routine testing of all pregnant women is costly and the need for testing should therefore be evaluated on a case-by-case basis.

Serologic testing edit

The enzyme-linked immunosorbent assay (or ELISA) is the most commonly available serologic test for measuring antibody to CMV. The result can be used to determine if acute infection, prior infection, or passively acquired maternal antibody in an infant is present. Other tests include various fluorescence assays, indirect hemagglutination, (PCR) and latex agglutination.[58][59]

An ELISA technique for CMV-specific IgM is available, but may give false-positive results unless steps are taken to remove rheumatoid factor or most of the IgG antibody before the serum sample is tested. Because CMV-specific IgM may be produced in low levels in reactivated CMV infection, its presence is not always indicative of primary infection. Only virus recovered from a target organ, such as the lung, provides unequivocal evidence that the current illness is caused by acquired CMV infection. If serologic tests detect a positive or high titer of IgG, this result should not automatically be interpreted to mean that active CMV infection is present. Active CMV infection is considered to be present if antibody tests of paired serum samples show a fourfold rise in IgG antibody and a significant level of IgM antibody (equal to at least 30% of the IgG value), or if virus is cultured from a urine or throat specimen.[citation needed]

Relevance to blood donors edit

Although the risks discussed above are generally low, CMV assays are part of the standard screening for non-directed blood donation (donations not specified for a particular person) in the U.S., the UK and many other countries. CMV-negative donations are then earmarked for transfusion to infants or people who are immunocompromised. Some blood donation centers maintain lists of donors whose blood is CMV negative due to special demands.[60]

Relevance to bone marrow donors edit

During allogeneic hematopoietic stem cell transplant, it is generally advised to match the serostatus of donor and recipient. If the recipient is seronegative, a seropositive donor carries a risk of de novo infection. Conversely, a seropositive recipient is at risk of viral reactivation if they receive a transplant from a seronegative donor, losing their innate defenses in the process. In general, the risk is highest for CMV seropositive recipients, in which viral reactivation is a cause of significant morbidity. For these reasons, CMV serologic testing is routine for both bone marrow donors and recipients.[61][62]

Prevention edit

Vaccination edit

Main article: Cytomegalovirus vaccine

A phase 2 study of a CMV-vaccine published in 2009 indicated an efficacy of 50%—the protection provided was limited, and a number of subjects contracted CMV infection despite vaccination. In one case also congenital CMV was encountered.[63]

In 2013, Astellas Pharma started on individuals who received a hematopoietic stem cell transplant a phase 3 trial with its CMV deoxyribonucleic acid DNA cytomegalovirus vaccine ASP0113.[64]

In 2015, Astellas Pharma commenced on healthy volunteers a phase 1 trial with its cytomegalovirus vaccine ASP0113.[65]

Further cytomegalovirus vaccines candidates are the CMV-MVA Triplex vaccine and the CMVpp65-A*0201 peptide vaccine. Both vaccine candidates are sponsored by the City of Hope National Medical Center. As of 2016, the development is in clinical phase 2 trial stage.[66][67]

Hygiene edit

The Centers for Disease Control and Prevention (CDC) recommend regular hand washing,[68] especially after changing diapers.[69] Hand washing is also recommended after feeding a child, wiping a child's nose or mouth, or handling children's toys.[70]

Treatment edit

Hyperimmune globulin enriched for CMV (CMV-IGIV) is an immunoglobulin G (IgG) containing a standardized number of antibodies to cytomegalovirus. It may be used for the prophylaxis of cytomegalovirus disease associated with transplantation of kidney, lung, liver, pancreas, and heart. Alone or in combination with an antiviral agent, it has been shown to:

  • Reduce the risk of CMV-related disease and death in some of the highest-risk transplant recipients
  • Provide a measurable long-term survival benefit
  • Produce minimal treatment-related side effects and adverse events.[71]

Ganciclovir (Cytovene) treatment is used for people with depressed immunity who have either sight-related or life-threatening illnesses. Valganciclovir (Valcyte) is an antiviral drug that is also effective and is given orally: it is a pro-drug that gets converted into ganciclovir in the body, but is much better absorbed orally than the latter. The therapeutic effectiveness is frequently compromised by the emergence of drug-resistant virus isolates. A variety of amino acid changes in the UL97 protein kinase and the viral DNA polymerase have been reported to cause drug resistance. Foscarnet or cidofovir are only given to people with CMV resistant to ganciclovir, because foscarnet has notable nephrotoxicity, resulting in increased or decreased Ca2+ or PO43−, and decreased Mg2+ levels.[72][73]

Letermovir has been approved by the European Medicines Agency[74] and the FDA[75] for treatment and prophylaxis of HCMV infection.

Drug resistance edit

 
Antiviral mechanisms of HCMV drugs.

All three currently licensed anti-HCMV drugs target the viral DNA polymerase, pUL54. Ganciclovir (GCV) acts as nucleoside analogue. Its antiviral activity requires phosphorylation by the HCMV protein kinase, pUL97.[76] The second drug, Cidofovir (CDV), is a nucleotide analogue, which is already phosphorylated and thus active. Finally, Foscarnet (FOS) has a different mode of action. It directly inhibits polymerase function by blocking the pyrophosphate binding site of pUL54 (note: investigational drug letermovir acts through a mechanism that involves viral terminase).[77] Two HCMV proteins are implicated in antiviral resistance against these three drugs: pUL97 and pUL54. Specific mutations in pUL97 can cause reduced phosphorylation activity of this viral protein kinase. Thus, fewer monophosphorylated – and thus active – GCV can be synthesized,[78] leading to antiviral resistance against GCV. About 90% of all GCV resistances are caused by such mutations in UL97.[79] Mutations in pUL54 may have different effects leading to antiviral drug resistance: A. They can lead to decreased affinity to antiviral compounds. This resistance mechanism concerns GCV, CDV and FOS and may lead to multidrug resistance.[80] B. Some mutations in pUL54 can increase the polymerase's exonuclease activity. This causes enhanced recognition of incorporated GCV and CDV. As a result, these dNTP analogues are excised more efficiently. Major risk factors for HCMV drug resistance are the residual capacity of the host's immune system to control viral replication and the overall amount and duration of viral replication.[81] HCMV antiviral drug resistance can be detected by phenotypic or by genotypic drug resistance testing. Phenotypic resistance testing involves cultivation of the virus in cell culture and testing its susceptibility using different antiviral drug concentrations in order to determine EC50 values. In contrast, genotypic resistance testing means the detection of resistance associated mutations in UL97 and UL54 by sequencing. Genotypic resistance testing is becoming the method of choice because it is faster, but requires previous phenotypic characterisation of each newly found mutation. This can be performed via a web-based search tool that links a person's HCMV sequence to a database containing all published UL97 and UL54 mutations and corresponding antiviral drug susceptibility phenotypes.[82]

Epidemiology edit

In the United States, CMV infection rises with age from about 60% of people infected by 6 years of age[34] leveling off at about 85–90% of the population by ages 75–80.[83]

See also edit

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November 27, 2023
human, betaherpesvirus, hcmv, redirects, here, airport, with, same, icao, code, burao, airport, also, called, human, cytomegalovirus, hcmv, species, virus, genus, cytomegalovirus, which, turn, member, viral, family, known, herpesviridae, herpesviruses, also, c. HCMV redirects here For the airport with the same ICAO code see Burao Airport Human betaherpesvirus 5 also called human cytomegalovirus HCMV 2 is species of virus in the genus Cytomegalovirus which in turn is a member of the viral family known as Herpesviridae or herpesviruses It is also commonly called CMV 3 Within Herpesviridae HCMV belongs to the Betaherpesvirinae subfamily which also includes cytomegaloviruses from other mammals 4 CMV is a double stranded DNA virus 5 Human cytomegalovirusSpecialtyInfectious diseaseCausesHuman betaherpesvirus 5Human betaherpesvirus 5CMV infection of a human lung pneumocyteVirus classification unranked VirusRealm DuplodnaviriaKingdom HeunggongviraePhylum PeploviricotaClass HerviviricetesOrder HerpesviralesFamily OrthoherpesviridaeGenus CytomegalovirusSpecies Human betaherpesvirus 5Synonyms 1 Human herpesvirus 5Although they may be found throughout the body HCMV infections are frequently associated with the salivary glands 4 HCMV infection is typically unnoticed in healthy people but can be life threatening for the immunocompromised such as HIV infected persons organ transplant recipients or newborn infants 3 Congenital cytomegalovirus infection can lead to significant morbidity and even death After infection HCMV remains latent within the body throughout life and can be reactivated at any time Eventually it may cause mucoepidermoid carcinoma and possibly other malignancies 6 such as prostate cancer 7 and breast cancer 8 HCMV is found in all geographic locations and all socioeconomic groups and infects between 60 and 70 of adults in the first world and almost 100 in the third world 9 Of all herpes viruses HCMV harbors the most genes dedicated to altering evading innate and adaptive host immunity and represents a lifelong burden of antigenic T cell surveillance and immune dysfunction 10 Commonly it is indicated by the presence of antibodies in the general population 3 Seroprevalence is age dependent 58 9 of individuals aged 6 and older are infected with CMV while 90 8 of individuals aged 80 and older are positive for HCMV 11 HCMV is also the virus most frequently transmitted to a developing fetus 12 HCMV infection is more widespread in developing countries and in communities with lower socioeconomic status and represents the most significant viral cause of birth defects in industrialized countries Congenital HCMV is the leading infectious cause of deafness learning disabilities and intellectual disability in children 13 CMV also seems to have a large impact on immune parameters in later life and may contribute to increased morbidity and eventual mortality 14 Contents 1 Signs and symptoms 2 Virology 2 1 Transmission 2 2 Replication 3 At risk populations 3 1 Pregnancy and congenital infection 3 2 Immunocompromised adults 3 3 Immunocompetent adults 4 Pathogenesis 5 Diagnosis 5 1 Serologic testing 5 2 Relevance to blood donors 5 3 Relevance to bone marrow donors 6 Prevention 6 1 Vaccination 6 2 Hygiene 7 Treatment 7 1 Drug resistance 8 Epidemiology 9 See also 10 References 11 External linksSigns and symptoms editHuman betaherpesvirus 5 infection has a classic triad of symptoms fever peaking in the late afternoon or early evening pharyngitis usually exudative and symmetrical adenopathy 15 16 17 Virology editTransmission edit The mode of HCMV transmission from person to person is unknown but is presumed to occur through bodily fluids including saliva urine blood and tears 18 Cytomegalovirus is most commonly transmitted through kissing and sexual intercourse It can also be transferred from an infected mother to her unborn child 4 Infection requires close intimate contact with a person secreting the virus in their saliva urine or other bodily fluids CMV can be transmitted sexually and via breast milk and also occurs through receiving transplanted organs or blood transfusions 19 Although HCMV is not highly contagious it has been shown to spread in households and among young children in day care centers 3 Replication edit HCMV replicates within infected endothelial cells 20 at a slow rate taking about five days in cell culture 21 It also infects fibroblasts which requires expression of only a trimeric viral receptor complex rather than the full pentameric complex that is required for infection of endothelial and epithelial cells 22 Like other herpesviruses HCMV expresses genes in a temporally controlled manner 23 24 Immediate early genes 0 4 hours after infection are involved in the regulation of transcription followed by early genes 4 48 hours after infection which are involved in viral DNA replication and further transcriptional regulation 23 Late genes are expressed during the remainder of infection up to viral egress and typically code for structural proteins While HCMV encodes for its own functional DNA polymerase the virus makes use of the host RNA polymerase for the transcription of all of its genes 25 In disseminated cytomegalovirus infections as may be seen in the context of an immunosuppressed host the virus is readily transmitted between polymorphonuclear leukocytes PM NLs and endothelial cells Infected endothelial cells produce cytokines that attract PM NLs which then adhere to the endothelium by interactions between their CD18 containing cell surface integrins and the endothelial expressed ICAM 1 Microfusions between the cells then take place in a manner dependent on expression of the viral gene locus UL128L 22 Synthesis of the viral double stranded DNA genome occurs at the host cell nucleus within specialized viral replication compartments 26 Nearly 75 of the genes encoded by HCMV strain AD169 can be deleted and still result in the production of infectious virus 27 This suggests that the virus focuses on avoiding the host immune system for a timely entrance into latency 28 At risk populations editCMV infections are most significant in the perinatal period and in people who are immunocompromised Pregnancy and congenital infection edit Main article Congenital cytomegalovirus infection HCMV is one of the vertically transmitted infections that lead to congenital abnormalities Others are Toxoplasmosis Rubella and Herpes simplex Congenital HCMV infection occurs when the mother has a primary infection during pregnancy 29 30 31 Up to 5 of every 1 000 live births are infected Five percent develop multiple handicaps and develop cytomegalic inclusion disease with nonspecific signs that resemble rubella Another five percent later develop cerebral calcification decreasing IQ levels dramatically and causing sensorineural deafness and psychomotor retardation citation needed However infants born preterm and infected with HCMV after birth may experience cognitive and motor impairments later in life 32 Immunocompromised adults edit CMV infection or reactivation in people whose immune systems are compromised for example people who have received transplants or are significantly burned causes illness and increases the risk of death 33 34 CMV reactivation is commonly seen in people with severe colitis 35 Specific disease entities recognized in those people are CMV hepatitis which may cause fulminant liver failure cytomegalovirus retinitis inflammation of the retina characterised by a pizza pie appearance on ophthalmoscopy cytomegalovirus colitis inflammation of the large bowel CMV pneumonitis CMV esophagitis 36 polyradiculopathy transverse myelitis and subacute encephalitisPeople without CMV infection who are given organ transplants from CMV infected donors require prophylactic treatment with valganciclovir ideally or ganciclovir and regular serological monitoring to detect a rising CMV titre if treated early establishment of a potentially life threatening infection can be prevented 37 Immunocompetent adults edit CMV infections can still be of clinical significance in adult immunocompetent populations 38 CMV mononucleosis some sources reserve mononucleosis for Epstein Barr virus only However the mononucleosis syndrome associated with CMV typically lacks signs of enlarged cervical lymph nodes and splenomegaly 39 18 CMV has also been associated with Guillain Barre syndrome 40 type 1 diabetes 41 and type 2 diabetes 42 The question of whether latent CMV infection has any negative effects on people who are otherwise healthy has been debated as of 2016 the answer was not clear but discussions had focused on whether latent CMV might increase the risk of some cardiovascular diseases and cancers 33 Pathogenesis edit nbsp Most healthy people who are infected by HCMV after birth have no symptoms 3 Some develop a syndrome similar to infectious mononucleosis or glandular fever 43 with prolonged fever and a mild hepatitis A sore throat is common After infection the virus remains latent in lymphocytes in the body for the rest of the person s life Overt disease rarely occurs unless immunity is suppressed either by drugs infection or old age Initial HCMV infection which often is asymptomatic is followed by a prolonged inapparent infection during which the virus resides in mononuclear cells without causing detectable damage or clinical illness 44 Infectious CMV may be shed in the bodily fluids of any infected person and can be found in urine saliva blood tears semen and breast milk The shedding of virus can occur intermittently without any detectable signs or symptoms nbsp Micrograph of CMV placentitis One cell on the image centre has the characteristic large nucleus with peri nuclear clearing Two cells centre right have the characteristic cytoplasmic viral inclusion bodies small pink globules H amp E stain CMV infection can be demonstrated microscopically by the detection of intranuclear inclusion bodies On H amp E staining the inclusion bodies stain dark pink and are called owl s eye inclusion bodies 45 HCMV infection is important to certain high risk groups 46 Major areas of risk of infection include pre natal or postnatal infants and immunocompromised individuals such as organ transplant recipients persons with leukemia or those infected with human immunodeficiency virus HIV In HIV infected persons HCMV is considered an AIDS defining infection indicating that the T cell count has dropped to low levels Lytically replicating viruses disrupt the cytoskeleton causing massive cell enlargement which is the source of the virus name A study published in 2009 links infection with CMV to high blood pressure in mice and suggests that the result of CMV infection of blood vessel endothelium in humans is a major cause of atherosclerosis 47 Researchers also found that when the cells were infected with CMV they created renin a protein known to contribute to high blood pressure Human CMV causes cellular senescence which could contribute to chronic inflammation inflammaging 48 Human CMV is also linked to age associated T cell dysfunction contributing to immunosenescence 48 COVID 19 symptom severity is associated with CMV although the exact mechanism has not been elucidated 49 CMV encodes a protein UL16 which is involved in the immune evasion of NK cell responses It binds to ligands ULBP1 ULBP2 and MICB of NK cell activating receptor NKG2D which prevents their surface expression These ligands are normally upregulated in times of cellular stress such as in viral infection and by preventing their upregulation CMV can prevent its host cell from dying due to NK cells 50 A substantial portion of the immune system is involved in continuously controlling CMV which drains the resources of the immune system 51 52 Death rates from infectious disease accelerate with age 53 and CMV infection correlates with reduced effectiveness of vaccination 54 Persons with the highest levels of CMV antibodies have a much higher risk of death from all causes compared with persons having few or no antibodies 55 56 Diagnosis editThis section does not cite any sources Please help improve this section by adding citations to reliable sources Unsourced material may be challenged and removed December 2009 Learn how and when to remove this template message nbsp Micrograph of CMV placentitis Most infections with CMV go undiagnosed as the virus usually produces few if any symptoms and tends to reactivate intermittently without symptoms Persons who have been infected with CMV develop antibodies to the virus which persist in the body for the lifetime of that individual A number of laboratory tests that detect these antibodies to CMV have been developed to determine if infection has occurred and are widely available from commercial laboratories In addition the virus can be cultured from specimens obtained from urine throat swabs bronchial lavages and tissue samples to detect active infection Both qualitative and quantitative polymerase chain reaction PCR testing for CMV are available as well allowing physicians to monitor the viral load of people infected with CMV The CMV pp65 antigenemia test is an immunofluorescence based assay which utilizes an indirect immunofluorescence technique for identifying the pp65 protein of cytomegalovirus in peripheral blood leukocytes 57 The CMV pp65 assay is widely used for monitoring CMV infection and its response to antiviral treatment in people who are under immunosuppressive therapy and have had renal transplantation surgery as the antigenemia results are obtained about 5 days before the onset of symptomatic CMV disease The advantage of this assay is the rapidity in providing results in a few hours and that the pp65 antigen determination represents a useful criterion for the physician to initiate antiviral therapy The major disadvantage of the pp65 assay is that only a limited number of samples can be processed per test batch CMV should be suspected if a person has symptoms of infectious mononucleosis but has negative test results for mononucleosis and Epstein Barr virus or if they show signs of hepatitis but have negative test results for hepatitis A B and C For best diagnostic results laboratory tests for CMV antibody should be performed by using paired serum samples One blood sample should be taken upon suspicion of CMV and another one taken within 2 weeks A virus culture can be performed any time the person is symptomatic Laboratory testing for antibodies to CMV can be performed to determine if a woman has already had CMV infection However routine testing of all pregnant women is costly and the need for testing should therefore be evaluated on a case by case basis Serologic testing edit The enzyme linked immunosorbent assay or ELISA is the most commonly available serologic test for measuring antibody to CMV The result can be used to determine if acute infection prior infection or passively acquired maternal antibody in an infant is present Other tests include various fluorescence assays indirect hemagglutination PCR and latex agglutination 58 59 An ELISA technique for CMV specific IgM is available but may give false positive results unless steps are taken to remove rheumatoid factor or most of the IgG antibody before the serum sample is tested Because CMV specific IgM may be produced in low levels in reactivated CMV infection its presence is not always indicative of primary infection Only virus recovered from a target organ such as the lung provides unequivocal evidence that the current illness is caused by acquired CMV infection If serologic tests detect a positive or high titer of IgG this result should not automatically be interpreted to mean that active CMV infection is present Active CMV infection is considered to be present if antibody tests of paired serum samples show a fourfold rise in IgG antibody and a significant level of IgM antibody equal to at least 30 of the IgG value or if virus is cultured from a urine or throat specimen citation needed Relevance to blood donors edit Although the risks discussed above are generally low CMV assays are part of the standard screening for non directed blood donation donations not specified for a particular person in the U S the UK and many other countries CMV negative donations are then earmarked for transfusion to infants or people who are immunocompromised Some blood donation centers maintain lists of donors whose blood is CMV negative due to special demands 60 Relevance to bone marrow donors edit During allogeneic hematopoietic stem cell transplant it is generally advised to match the serostatus of donor and recipient If the recipient is seronegative a seropositive donor carries a risk of de novo infection Conversely a seropositive recipient is at risk of viral reactivation if they receive a transplant from a seronegative donor losing their innate defenses in the process In general the risk is highest for CMV seropositive recipients in which viral reactivation is a cause of significant morbidity For these reasons CMV serologic testing is routine for both bone marrow donors and recipients 61 62 Prevention editVaccination edit Main article Cytomegalovirus vaccine A phase 2 study of a CMV vaccine published in 2009 indicated an efficacy of 50 the protection provided was limited and a number of subjects contracted CMV infection despite vaccination In one case also congenital CMV was encountered 63 In 2013 Astellas Pharma started on individuals who received a hematopoietic stem cell transplant a phase 3 trial with its CMV deoxyribonucleic acid DNA cytomegalovirus vaccine ASP0113 64 In 2015 Astellas Pharma commenced on healthy volunteers a phase 1 trial with its cytomegalovirus vaccine ASP0113 65 Further cytomegalovirus vaccines candidates are the CMV MVA Triplex vaccine and the CMVpp65 A 0201 peptide vaccine Both vaccine candidates are sponsored by the City of Hope National Medical Center As of 2016 the development is in clinical phase 2 trial stage 66 67 Hygiene edit The Centers for Disease Control and Prevention CDC recommend regular hand washing 68 especially after changing diapers 69 Hand washing is also recommended after feeding a child wiping a child s nose or mouth or handling children s toys 70 Treatment editHyperimmune globulin enriched for CMV CMV IGIV is an immunoglobulin G IgG containing a standardized number of antibodies to cytomegalovirus It may be used for the prophylaxis of cytomegalovirus disease associated with transplantation of kidney lung liver pancreas and heart Alone or in combination with an antiviral agent it has been shown to Reduce the risk of CMV related disease and death in some of the highest risk transplant recipients Provide a measurable long term survival benefit Produce minimal treatment related side effects and adverse events 71 Ganciclovir Cytovene treatment is used for people with depressed immunity who have either sight related or life threatening illnesses Valganciclovir Valcyte is an antiviral drug that is also effective and is given orally it is a pro drug that gets converted into ganciclovir in the body but is much better absorbed orally than the latter The therapeutic effectiveness is frequently compromised by the emergence of drug resistant virus isolates A variety of amino acid changes in the UL97 protein kinase and the viral DNA polymerase have been reported to cause drug resistance Foscarnet or cidofovir are only given to people with CMV resistant to ganciclovir because foscarnet has notable nephrotoxicity resulting in increased or decreased Ca2 or PO43 and decreased Mg2 levels 72 73 Letermovir has been approved by the European Medicines Agency 74 and the FDA 75 for treatment and prophylaxis of HCMV infection Drug resistance edit nbsp Antiviral mechanisms of HCMV drugs All three currently licensed anti HCMV drugs target the viral DNA polymerase pUL54 Ganciclovir GCV acts as nucleoside analogue Its antiviral activity requires phosphorylation by the HCMV protein kinase pUL97 76 The second drug Cidofovir CDV is a nucleotide analogue which is already phosphorylated and thus active Finally Foscarnet FOS has a different mode of action It directly inhibits polymerase function by blocking the pyrophosphate binding site of pUL54 note investigational drug letermovir acts through a mechanism that involves viral terminase 77 Two HCMV proteins are implicated in antiviral resistance against these three drugs pUL97 and pUL54 Specific mutations in pUL97 can cause reduced phosphorylation activity of this viral protein kinase Thus fewer monophosphorylated and thus active GCV can be synthesized 78 leading to antiviral resistance against GCV About 90 of all GCV resistances are caused by such mutations in UL97 79 Mutations in pUL54 may have different effects leading to antiviral drug resistance A They can lead to decreased affinity to antiviral compounds This resistance mechanism concerns GCV CDV and FOS and may lead to multidrug resistance 80 B Some mutations in pUL54 can increase the polymerase s exonuclease activity This causes enhanced recognition of incorporated GCV and CDV As a result these dNTP analogues are excised more efficiently Major risk factors for HCMV drug resistance are the residual capacity of the host s immune system to control viral replication and the overall amount and duration of viral replication 81 HCMV antiviral drug resistance can be detected by phenotypic or by genotypic drug resistance testing Phenotypic resistance testing involves cultivation of the virus in cell culture and testing its susceptibility using different antiviral drug concentrations in order to determine EC50 values In contrast genotypic resistance testing means the detection of resistance associated mutations in UL97 and UL54 by sequencing Genotypic resistance testing is becoming the method of choice because it is faster but requires previous phenotypic characterisation of each newly found mutation This can be performed via a web based search tool that links a person s HCMV sequence to a database containing all published UL97 and UL54 mutations and corresponding antiviral drug susceptibility phenotypes 82 Epidemiology editIn the United States CMV infection rises with age from about 60 of people infected by 6 years of age 34 leveling off at about 85 90 of the population by ages 75 80 83 See also editHerpesviridae Epstein Barr virus one of the most common viruses in humans References edit Davison Andrew 27 January 2016 Rename species in the family Herpesviridae to incorporate a subfamily designation PDF International Committee on Taxonomy of Viruses ICTV Retrieved 13 March 2019 taxonomy Taxonomy browser Human betaherpesvirus 5 www ncbi nlm nih gov Retrieved 25 July 2020 a b c d e Ryan KJ Ray CG eds 2004 Sherris Medical Microbiology 4th ed McGraw Hill pp 556 566 9 ISBN 978 0 8385 8529 0 a b c Koichi Yamanishi Arvin Ann M Gabriella Campadelli Fiume Edward Mocarski Moore Patrick Roizman Bernard Whitley Richard 2007 Human herpesviruses biology therapy and immunoprophylaxis Cambridge UK Cambridge University Press ISBN 978 0 521 82714 0 Zanella M Cordey S Kaiser L 2020 Beyond Cytomegalovirus and Epstein Barr Virus a Review of Viruses Composing the Blood Virome of Solid Organ Transplant and Hematopoietic Stem Cell Transplant Recipients Clinical Microbiology Reviews 33 4 e00027 20 doi 10 1128 CMR 00027 20 PMC 7462738 PMID 32847820 Melnick M Sedghizadeh PP Allen CM Jaskoll T 10 November 2011 Human cytomegalovirus and mucoepidermoid carcinoma of salivary glands cell specific localization of active viral and oncogenic signaling proteins is confirmatory of a causal relationship Experimental and Molecular Pathology 92 1 118 25 doi 10 1016 j yexmp 2011 10 011 PMID 22101257 S2CID 41446671 Geder L Sanford EJ Rohner TJ Rapp F 1977 Cytomegalovirus and cancer of the prostate in vitro transformation of human cells Cancer Treat Rep 61 2 139 46 PMID 68820 Kumar Amit Tripathy Manoj Kumar Pasquereau Sebastien Al Moussawi Fatima Abbas Wasim Coquard Laurie Khan Kashif Aziz Russo Laetitia Algros Marie Paule Valmary Degano Severine Adotevi Olivier April 2018 The Human Cytomegalovirus Strain DB Activates Oncogenic Pathways in Mammary Epithelial Cells eBioMedicine 30 167 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Curlie Cytomegalovirus CMV US Centers for Disease Control and Prevention CDC 22 May 2009 HCMV drug resistance mutations tool Human herpesvirus 5 NCBI Taxonomy Browser 10359 Retrieved from https en wikipedia org w index php title Human betaherpesvirus 5 amp oldid 1183265733, wikipedia, wiki, book, books, library,

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