Arbovirus Reports 2015

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Arbovirus Reports Arboviruses (Arthropod-borne) are a group of viral infections transmitted by the bite of arthropods, most commonly mosquitoes. Some of these infections are endemic; others may be imported into Australia following travel to endemic areas. Where a competent local mosquito vector exists there is always concern regarding the introduction of new endemic viruses into Australia as occurs frequently in North Queensland with recurrent dengue introductions and subsequent outbreaks. This report will summarise results of testing for various arboviruses at Sullivan Nicolaides Pathology (SNP). Whilst most samples come from Queensland, the laboratory also serves as a reference laboratory for some other Sonic Laboratories located around Australia. A non-exhaustive list of mosquito borne viruses of interest are listed: Alphaviruses Flaviviruses Ross River Virus Endemic Fever Rash & Arthralgia Barmah Forest Virus Endemic Fever Rash & Arthralgia Chikungunya Virus Exotic Fever Rash & Arthralgia Sindbus Virus Endemic Fever Vesicular Rash & Arthralgia Dengue Kunjin virus (related to West Nile Virus) Repeated outbreaks locally in Far North Queensland Endemic Fever & Rash Fever & Encephalitis Murray Valley Encephalitis Virus Endemic Fever & Encephalitis Japanese B Encephalitis virus Torres Strait & FNQ Fever & Encephalitis Zika virus Exotic Fever Rash & Arthralgia These infections are usually diagnosed serologically by the detection of antibodies in blood. Following a short but variable incubation period and another week after onset of symptoms, the infected individual develops an immune response characterized by specific IgM. Five to ten days later, specific IgG appears. Early in the illness, prior to the development of IgM, a short lived viraemia occurs. There is no PCR or antigen test available to detect this early viraemia in clinical diagnostic laboratories at this point in time, although this is available in reference laboratories. With resolution of acute infection the specific IgG persists for life. Usually IgM antibodies becomes undetectable in approximately 3-6 months.

Arbovirus Reports Depending upon the timing of the blood collection in relation to symptoms an infected individual may test: IgG Negative; IgM Negative (NN): No evidence of acute or past infection Acute sample in the first week of clinical illness prior to development of any antibodies Repeat convalescent testing is indicated IgG Negative; IgM Positive (NP): Presumptive infection should be considered in the correct clinical context Early in the acute illness prior to development of IgG Note that detection of IgM alone can be misleading and may represent a False positive nonspecific IgM Cross reaction due to another infection.e.g CMV, EBV, Parvovirus In this case IgM reactivity to a number of infectious agents may be present It is always wise to confirm true infection by collection of a convalescent sample in 7-14 days If true infection is present a seroconversion for specific IgG will occur (PP) IgG Positive; IgM Positive (PP): This usually indicates recent acute infection BUT even this is not fool proof Specific IgM may persist for months to years following acute infection Note that this persistence does not indicate ongoing chronic infection Intercurrent infection with another virus can result in a transient anamnestic IgM response It is helpful to review any previous serological results to clarify the true situation Seroconversion: (NN or NP to PP) Change from RRV IgG negative to RRV IgG positive between acute and convalescent samples This is the definitive confirmation of acute infection Significant change in antibody level or titre (NP or PP to PP): Convalescent samples are often requested to test in parallel This is most useful when the initial IgG is negative Whilst changes in the absorbance (degree of positivity) can be obvious when samples are tested in parallel, enzyme immunoassays (EIAs) are not titred, and it may be difficult to determine what constitutes significant. This is generally not determined or validated for individual EIAs and often represents the microbiologists interpretation of the clinical scenario together with results from other test results that may be cross reacting The classification of results is complicated by an Equivocal range (E) which is a grey area between Negative (N) and Positive (P) for both IgG and IgM. Acute cases in this summary are identified as the first occurrence of IgG Positive IgM Positive (PP) for a given individual in our data base dating back to 1999 or evidence of a seroconversion. (NN, NE, NP, to EP, PE, EE ). There are major limitations as the patient may not always be tested in the same laboratory and the patterns of referral are quite variable. An NN summary result indicates the % susceptibility in the test population for the specific virus. A PN (plus EN) summary result provides an indication of those with past infection for the tested population. Page: 2

Barmah Forest Report *Acute Cases - First Instance of IgG Pos, IgM Pos (PP) in SNP database since 1999. Page: 3

Ross River Report *Acute Cases - First Instance of IgG Pos, IgM Pos (PP) in SNP database since 1999. Page: 4

Chikungunya Report *Acute Cases - First Instance of IgG Pos, IgM Pos (PP) in SNP database since testing was first instituted in 2013 Page: 5

Key Key IgG/IgM Description PP EP EE NP NE PE PN EN NN IgG = Positive, IgM = Positive IgG = Equivocal, IgM = Positive IgG = Equivocal, IgM = Equivocal IgG = Negative, IgM = Positive IgG = Negative, IgM = Equivocal IgG = Positive, IgM = Equivocal IgG = Positive, IgM = Negative IgG =Equivocal, IgM = Negative IgG = Negative, IgM = Negative Page: 6