Both a low initial CD4 cell count and a high HIV DNA level are predictive of rapid progression of untreated primary HIV-1 infection. Affected patients may therefore benefit from close clinical and laboratory monitoring and/or early administration of treatment.
Inherited red blood cell (RBC) membrane disorders, such as hereditary
spherocytosis, elliptocytosis and hereditary ovalocytosis, result from mutations
in genes encoding various RBC membrane and skeletal proteins. The RBC membrane,
a composite structure composed of a lipid bilayer linked to a
spectrin/actin-based membrane skeleton, confers upon the RBC unique features of
deformability and mechanical stability. The disease severity is primarily
dependent on the extent of membrane surface area loss. RBC membrane disorders
can be readily diagnosed by various laboratory approaches that include RBC
cytology, flow cytometry, ektacytometry, electrophoresis of RBC membrane
proteins and genetics. The reference technique for diagnosis of RBC membrane
disorders is the osmotic gradient ektacytometry. However, in spite of its
recognition as the reference technique, this technique is rarely used as a
routine diagnosis tool for RBC membrane disorders due to its limited
availability. This may soon change as a new generation of ektacytometer has been
recently engineered. In this review, we describe the workflow of the samples
shipped to our Hematology laboratory for RBC membrane disorder analysis and the
data obtained for a large cohort of French patients presenting with RBC membrane
disorders using a newly available version of the ektacytomer.
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