PLoS ONE (Jan 2020)

Sickle cell disease: A distinction of two most frequent genotypes (HbSS and HbSC).

  • Caroline Conceição da Guarda,
  • Sètondji Cocou Modeste Alexandre Yahouédéhou,
  • Rayra Pereira Santiago,
  • Joelma Santana Dos Santos Neres,
  • Camila Felix de Lima Fernandes,
  • Milena Magalhães Aleluia,
  • Camylla Vilas Boas Figueiredo,
  • Luciana Magalhães Fiuza,
  • Suellen Pinheiro Carvalho,
  • Rodrigo Mota de Oliveira,
  • Cleverson Alves Fonseca,
  • Uche Samuel Ndidi,
  • Valma Maria Lopes Nascimento,
  • Larissa Carneiro Rocha,
  • Marilda Souza Goncalves

DOI
https://doi.org/10.1371/journal.pone.0228399
Journal volume & issue
Vol. 15, no. 1
p. e0228399

Abstract

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Sickle cell disease (SCD) consists of a group of hemoglobinopathies in which individuals present highly variable clinical manifestations. Sickle cell anemia (SCA) is the most severe form, while SC hemoglobinopathy (HbSC) is thought to be milder. Thus, we investigated the clinical manifestations and laboratory parameters by comparing each SCD genotype. We designed a cross-sectional study including 126 SCA individuals and 55 HbSC individuals in steady-state. Hematological, biochemical and inflammatory characterization was performed as well as investigation of previous history of clinical events. SCA patients exhibited most prominent anemia, hemolysis, leukocytosis and inflammation, whereas HbSC patients had increased lipid determinations. The main cause of hospitalization was pain crises on both genotypes. Vaso-occlusive events and pain crises were associated with hematological, inflammatory and anemia biomarkers on both groups. Cluster analysis reveals hematological, inflammatory, hemolytic, endothelial dysfunction and anemia biomarkers in HbSC disease as well as SCA. The results found herein corroborate with previous studies suggesting that SCA and HbSC, although may be similar from the genetic point of view, exhibit different clinical manifestations and laboratory alterations which are useful to monitor the clinical course of each genotype.