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Open Access 01-12-2018 | Research article

A ten year review of the sickle cell program in Muhimbili National Hospital, Tanzania

Authors: Julie Makani, Furahini Tluway, Abel Makubi, Deogratius Soka, Siana Nkya, Raphael Sangeda, Josephine Mgaya, Stella Rwezaula, Fenella J. Kirkham, Christina Kindole, Elisha Osati, Elineema Meda, Robert W. Snow, Charles R. Newton, David Roberts, Muhsin Aboud, Swee Lay Thein, Sharon E. Cox, Lucio Luzzatto, Bruno P. Mmbando

Published in: BMC Hematology | Issue 1/2018

Abstract

Background

Africa has the highest burden of Sickle cell disease (SCD) but there are few large, systematic studies providing reliable descriptions of the disease spectrum. Tanzania, with 11,000 SCD births annually, established the Muhimbili Sickle Cell program aiming to improve understanding of SCD in Africa. We report the profile of SCD seen in the first 10 years at Muhimbili National Hospital (MNH).

Methods

Individuals seen at MNH known or suspected to have SCD were enrolled at clinic and laboratory testing for SCD, haematological and biochemical analyses done. Ethnicity was self-reported. Clinical and laboratory features of SCD were documented. Comparison was made with non-SCD population as well as within 3 different age groups (< 5, 5–17 and ≥ 18 years) within the SCD population.

Results

From 2004 to 2013, 6397 individuals, 3751 (58.6%) SCD patients, were enrolled, the majority (47.4%) in age group 5–17 years. There was variation in the geographical distribution of SCD. Individuals with SCD compared to non-SCD, had significantly lower blood pressure and peripheral oxygen saturation (SpO₂). SCD patients had higher prevalence of severe anemia, jaundice and desaturation (SpO₂ < 95%) as well as higher levels of reticulocytes, white blood cells, platelets and fetal hemoglobin. The main causes of hospitalization for SCD within a 12-month period preceding enrolment were pain (adults), and fever and severe anemia (children). When clinical and laboratory features were compared in SCD within 3 age groups, there was a progressive decrease in the prevalence of splenic enlargement and an increase in prevalence of jaundice. Furthermore, there were significant differences with monotonic trends across age groups in SpO2, hematological and biochemical parameters.

Conclusion

This report confirms that the wide spectrum of clinical expression of SCD observed elsewhere is also present in Tanzania, with non-uniform geographical distribution across the country. Age-specific analysis is consistent with different disease-patterns across the lifespan.

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Title: A ten year review of the sickle cell program in Muhimbili National Hospital, Tanzania
Authors: Julie Makani
Furahini Tluway
Abel Makubi
Deogratius Soka
Siana Nkya
Raphael Sangeda
Josephine Mgaya
Stella Rwezaula
Fenella J. Kirkham
Christina Kindole
Elisha Osati
Elineema Meda
Robert W. Snow
Charles R. Newton
David Roberts
Muhsin Aboud
Swee Lay Thein
Sharon E. Cox
Lucio Luzzatto
Bruno P. Mmbando
Publication date: 01-12-2018
Publisher: BioMed Central
Published in: BMC Hematology / Issue 1/2018
Electronic ISSN: 2052-1839
DOI: https://doi.org/10.1186/s12878-018-0125-0

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