In the study region, the first semester coincides with the rainy season and is considered seasonally epidemic for arboviruses and contributes significantly to the proliferation and development of Aedes aegypti [4]. One donor was found positive for CHIKV and one for DENV. CHIKV was found in a non-epidemic period and had an estimated prevalence of 0.02%, which suggests that in non-epidemic periods, the chances of blood donors being able to transmit the virus, as they are asymptomatic or symptomatic, after donation, may be increased. DENV in an epidemic period with an annual prevalence of 0.01%. Both prevalence’s match or are higher than those found for the Hepatitis C virus (0.01%) and for the Hepatitis B virus (0.02%) in the study region (Table 1). The detection of a positive case of DENV was found in the first semester of 2019, the period of greatest circulation of the vectors of the disease, and the period in which almost all cases occur in Brazil [5], suggesting attention in relation to this agent.
As for CHIKV in 2009, during an epidemic in a province in Thailand, a prevalence of 0.03% was found in blood donors, such as our study (6). So far, in the world literature, it has not been possible to predict transfusion transmission of this virus. DENV is an agent recognized as a threat to transfusion safety (7) as examples of studies carried out in other countries, including Brazil, where the transmission of blood transfusion with recipients in conditions of development is known to worsen the disease, compromising the primary treatment that the patient was receiving [1, 8].
As for ZIKAV, a systematic review found a prevalence of 0.85% of the virus in blood donors, although the development of apparent symptoms of the disease by ZIKAV in blood component containers has not been proven [8]. As far as we know, there are no descriptions of prevalence in the northern region of Brazil and, in this study, we did not detect this virus in blood donors. Positive donors for DENV and CHIKV were contacted by the project team and after clinical evaluation were classified as symptomatic after donation, however, both had mild symptoms such as mild fever, malaise, body aches, tiredness and both did not seek medical attention. at the time of donation. In this research, blood donations positive for DENV and CHIKV had no recipients.
The positive DENV and CHIKV samples were simulated in different sample pool quantities, up to the amount of 14 samples in the pool (Table 2). Was observed that if the DENV positive sample had been carried out within a plasma pool of 14 donation samples, it would have been detected automatically in the system protocol, however even in a pool of 20 samples it could be detected by the operator of the device, given that there was a curve growth (amplification of viral cDNA). As for CHIKV, it was observed that even if this sample were composing a pool of 20 plasma samples, it would have been detected automatically by the system protocol.
We conclude the need for continuous monitoring of research for ZIKAV and CHIKV and there is a need to include a continuous and mandatory molecular screening test for the four subtypes of DENV in the routine of blood centers, preventing this agent from being transmitted to recipients of blood components, and that special groups of immunosuppressed receptors may die.