Controlling Sickle Cell Disease in Ghana--ethics and options
- PMID: 22187596
- PMCID: PMC3282939
- DOI: 10.4314/pamj.v10i0.72223
Controlling Sickle Cell Disease in Ghana--ethics and options
Abstract
Sickle Cell Disease (SCD) is a significant public health burden in Ghana. Recent studies indicate that 2% of Ghanaian newborns are affected by SCD; one in three Ghanaians has the hemoglobin S and/or C gene. As a means of controlling the disease, some authorities have recommended prenatal diagnosis (PND) and selective abortion. In the current era, SCD has a good prognosis and fairly reasonable quality of life. Advances in bone marrow transplantation have shown the disease is curable in selected patients. PND and selective abortion therefore raises a myriad of ethical dilemmas which are considered in this review. In the light of the demonstration of improved prognosis in recent times, PND and selective abortion appears to be applying capital punishment to the unborn child for "crimes" only the parents can be responsible for. In this review, we recommend control of SCD on three levels--preconception genetic testing and strategic reproductive choices, PND and education for carrier parents, and holistic management of persons with SCD. We emphasize the critical importance of self-management, especially self-awareness, in assuring a good quality of life for persons with SCD. We believe such an approach is cost-effective, and consistent with sound ethical principles and good conscience.
References
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- Ohene-Frempong K, Oduro J, Tetteh H, Nkrumah F. Screening newborns for sickle cell disease in Ghana. Pediatrics. 2008;121(Suppl 2):S120–S121.
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- Ghana Health Service-Non-Communicable Diseases Control Programme. Disease Control and Prevention Department. Strategic Framework for the Management. Prevention and Control of Sickle Cell Disease in Ghana (Draft) 11th March 2010.
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- 30 yr old male with sickle cell anemia. interview by author (Edwin, AK); Accra, Ghana, 26th March 2010.
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- Pain in sickle cell disease. Rates and risk factors. N Engl J Med. 1991;325:11–16. - PubMed
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