Revista Brasileira de Ginecologia e Obstetrícia. 2024;46:e-rbgo88
Recent evidence demonstrates na increase in negative maternal and neonatal outcomes in cases of SARS-CoV-2 infection, such as greater severity of the disease, need for mechanical ventilation and longer hospitalization in intensive care units.(,) The greater severity of infectious diseases in pregnancy occurs due to anatomical and immunological changes, such as a change in the CD4 cell phenotype from the TH2 subgroup to TH1, a decrease in the function of natural killer cells and a reduction in plasma cell dendritic cells, with the first and third trimesters of pregnancy being the periods of greatest inflammatory activity and susceptibility to diseases.() Furthermore, there are obstetric and neonatal impacts associated with COVID-19 infection during pregnancy, such as premature rupture of ovular membranosa, prematurity, fetal distress, increased number of cesarean sections, tachypnea, neonatal sepsis and death maternal.(,)
COVID-19 infection can also cause damage to the placenta, especially if it comes from the delta variant. It is known that COVID requires ACE II and TMPRSS2 receptors to initiate and facilitate infection, but these receptors are poorly expressed in placental cells, which reduces the structural damage caused by the disease.() However, this factor does not prevent disease. Placental, since signs of maternal-fetal vascular malperfusion, zones of avascular villi, villous thrombi and infarction and villous edema can be observed.() In addition to histiocytic intervillositis, deposition of perivillous or subchorionic fibrin, trophoblastic necrosis and increased incidence chorangiosis.() These changes are mainly due to cellular reactions caused by the death of the virus, the action of anti-SARS-CoV antibodies, the local inflammatory process and syncytiotrophoblastic ischemia, without necessarily having a placental infection.()
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Recent evidence demonstrates na increase in negative maternal and neonatal outcomes in cases of SARS-CoV-2 infection, such as greater severity of the disease, need for mechanical ventilation and longer hospitalization in intensive care units.(,) The greater severity of infectious diseases in pregnancy occurs due to anatomical and immunological changes, such as a change in the CD4 cell phenotype from the TH2 subgroup to TH1, a decrease in the function of natural killer cells and a reduction in plasma cell dendritic cells, with the first and third trimesters of pregnancy being the periods of greatest inflammatory activity and susceptibility to diseases.() Furthermore, there are obstetric and neonatal impacts associated with COVID-19 infection during pregnancy, such as premature rupture of ovular membranosa, prematurity, fetal distress, increased number of cesarean sections, tachypnea, neonatal sepsis and death maternal.(,)
COVID-19 infection can also cause damage to the placenta, especially if it comes from the delta variant. It is known that COVID requires ACE II and TMPRSS2 receptors to initiate and facilitate infection, but these receptors are poorly expressed in placental cells, which reduces the structural damage caused by the disease.() However, this factor does not prevent disease. Placental, since signs of maternal-fetal vascular malperfusion, zones of avascular villi, villous thrombi and infarction and villous edema can be observed.() In addition to histiocytic intervillositis, deposition of perivillous or subchorionic fibrin, trophoblastic necrosis and increased incidence chorangiosis.() These changes are mainly due to cellular reactions caused by the death of the virus, the action of anti-SARS-CoV antibodies, the local inflammatory process and syncytiotrophoblastic ischemia, without necessarily having a placental infection.()
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