Malaria in Children with Sickle Cell Anaemia in Areas with Low, Moderate and High Transmission in Uganda

Ruth Namazzi; Richard Idro; Dennis Kalibala; John Ssenkusu; Pamela Akun; Vincent Mboizi; Thandile Nkosi Gondwe; Deogratias Munube; Philip Kasirye; Catherine Nabaggala; Chandy C. John; Nancy S. Green; Bjarne Robberstat; Boele van Hensbroek; Feiko Ter Kuile; Kamija S. Phiri; Robert Opoka

doi:10.1182/blood-2023-189066

Abstract

Background. Few large prospective studies have evaluated burden and outcomes of malaria in children with sickle cell anaemia (SCA) in malaria endemic countries. We evaluated the incidence, complications and outcome of malaria in three cohorts of Ugandan children with SCA in three areas with differing malaria transmission.

Methods. Cohort 1 were SCA aged 3-9 years, enrolled in the hydroxyurea therapy for neurological and cognitive protection in Uganda (BRAINSAFE II) trial at Mulago Hospital, a low transmission area, while cohort 2 and 3 aged 6 months to 15 years, were enrolled in the dihydroartemisinin-piperaquine (DP) or sulphadoxine-pyrimethamine (SP) for the chemoprevention of malaria in SCA (CHEMCHA) trial at Jinja Hospital (moderate transmission) and Kitgum Hospital (high transmission). In cohort 1, all received SP for malaria chemoprophylaxis and hydroxyurea at 20-30mg/kg/day, while cohorts 2 and 3, received either DP or SP for malaria chemoprevention, and a proportion (10%) received hydroxyurea in the study.

Results. A total of 706 participants were enrolled: 267, 249 and 190 at Mulago, Jinja and Kitgum respectively. The mean age was 6.5 (SD 3.4) years; 5.1 (1.7), 7.9 (4.3) and 6.8 (3.5) years for Mulago, Jinja, and Kitgum respectively. Incidence of malaria was 13 (95% CI 6, 20) per 100 child years in low, 38 (95% CI 26, 51) in moderate and 104 (95% CI 64, 144) in the high transmission area, p<0.001. Adjusting for hydroxyurea treatment, incidence of malaria was 33 (95%CI 14, 52) per 100 child year on hydroxyurea and 51 (95%CI 40, 62) per 100 child years without hydroxyurea, p=0.001. The most common SCA-related complications were anaemia (39.6%, 133/336), and pain (27.7%, 93/336) among children with malaria. Over a period of 1042.8 person years, there were 115 admissions for malaria, with an overall incidence of 11 per 100 child year (95% CI 9, 13), and this differed across sites, p<0.001. Overall, 1.5% (11/706) children died, and 18.2% (2/11) deaths were directly related to malaria infection.

Conclusion. Malaria incidence remains high among Ugandan children with SCA, and differs by transmission patterns. Prevention strategies should be strengthened, especially in high transmission areas.

Original language	English
Pages (from-to)	5327
Number of pages	1
Journal	Blood
Volume	142
Issue number	S1
Early online date	2 Nov 2023
DOIs	https://doi.org/10.1182/blood-2023-189066
Publication status	Published - 2 Nov 2023
Event	65th ASH Annual Meeting - San Diego, United States Duration: 9 Dec 2023 → 12 Dec 2023

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10.1182/blood-2023-189066

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Namazzi, R., Idro, R., Kalibala, D., Ssenkusu, J., Akun, P., Mboizi, V., Gondwe, T. N., Munube, D., Kasirye, P., Nabaggala, C., John, C. C., Green, N. S., Robberstat, B., Hensbroek, B. V., Ter Kuile, F., Phiri, K. S., & Opoka, R. (2023). Malaria in Children with Sickle Cell Anaemia in Areas with Low, Moderate and High Transmission in Uganda. Blood, 142(S1), 5327. https://doi.org/10.1182/blood-2023-189066

@article{5112952e5cd445c4bdb31c5cc589823b,

title = "Malaria in Children with Sickle Cell Anaemia in Areas with Low, Moderate and High Transmission in Uganda",

abstract = "Background. Few large prospective studies have evaluated burden and outcomes of malaria in children with sickle cell anaemia (SCA) in malaria endemic countries. We evaluated the incidence, complications and outcome of malaria in three cohorts of Ugandan children with SCA in three areas with differing malaria transmission.Methods. Cohort 1 were SCA aged 3-9 years, enrolled in the hydroxyurea therapy for neurological and cognitive protection in Uganda (BRAINSAFE II) trial at Mulago Hospital, a low transmission area, while cohort 2 and 3 aged 6 months to 15 years, were enrolled in the dihydroartemisinin-piperaquine (DP) or sulphadoxine-pyrimethamine (SP) for the chemoprevention of malaria in SCA (CHEMCHA) trial at Jinja Hospital (moderate transmission) and Kitgum Hospital (high transmission). In cohort 1, all received SP for malaria chemoprophylaxis and hydroxyurea at 20-30mg/kg/day, while cohorts 2 and 3, received either DP or SP for malaria chemoprevention, and a proportion (10\%) received hydroxyurea in the study.Results. A total of 706 participants were enrolled: 267, 249 and 190 at Mulago, Jinja and Kitgum respectively. The mean age was 6.5 (SD 3.4) years; 5.1 (1.7), 7.9 (4.3) and 6.8 (3.5) years for Mulago, Jinja, and Kitgum respectively. Incidence of malaria was 13 (95\% CI 6, 20) per 100 child years in low, 38 (95\% CI 26, 51) in moderate and 104 (95\% CI 64, 144) in the high transmission area, p<0.001. Adjusting for hydroxyurea treatment, incidence of malaria was 33 (95\%CI 14, 52) per 100 child year on hydroxyurea and 51 (95\%CI 40, 62) per 100 child years without hydroxyurea, p=0.001. The most common SCA-related complications were anaemia (39.6\%, 133/336), and pain (27.7\%, 93/336) among children with malaria. Over a period of 1042.8 person years, there were 115 admissions for malaria, with an overall incidence of 11 per 100 child year (95\% CI 9, 13), and this differed across sites, p<0.001. Overall, 1.5\% (11/706) children died, and 18.2\% (2/11) deaths were directly related to malaria infection.Conclusion. Malaria incidence remains high among Ugandan children with SCA, and differs by transmission patterns. Prevention strategies should be strengthened, especially in high transmission areas.",

author = "Ruth Namazzi and Richard Idro and Dennis Kalibala and John Ssenkusu and Pamela Akun and Vincent Mboizi and Gondwe, \{Thandile Nkosi\} and Deogratias Munube and Philip Kasirye and Catherine Nabaggala and John, \{Chandy C.\} and Green, \{Nancy S.\} and Bjarne Robberstat and Hensbroek, \{Boele van\} and \{Ter Kuile\}, Feiko and Phiri, \{Kamija S.\} and Robert Opoka",

year = "2023",

month = nov,

day = "2",

doi = "10.1182/blood-2023-189066",

language = "English",

volume = "142",

pages = "5327",

journal = "Blood",

issn = "0006-4971",

publisher = "Elsevier B.V.",

number = "S1",

note = "65th ASH Annual Meeting ; Conference date: 09-12-2023 Through 12-12-2023",

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Namazzi, R, Idro, R, Kalibala, D, Ssenkusu, J, Akun, P, Mboizi, V, Gondwe, TN, Munube, D, Kasirye, P, Nabaggala, C, John, CC, Green, NS, Robberstat, B, Hensbroek, BV, Ter Kuile, F, Phiri, KS & Opoka, R 2023, 'Malaria in Children with Sickle Cell Anaemia in Areas with Low, Moderate and High Transmission in Uganda', Blood, vol. 142, no. S1, pp. 5327. https://doi.org/10.1182/blood-2023-189066

TY - JOUR

T1 - Malaria in Children with Sickle Cell Anaemia in Areas with Low, Moderate and High Transmission in Uganda

AU - Namazzi, Ruth

AU - Idro, Richard

AU - Kalibala, Dennis

AU - Ssenkusu, John

AU - Akun, Pamela

AU - Mboizi, Vincent

AU - Gondwe, Thandile Nkosi

AU - Munube, Deogratias

AU - Kasirye, Philip

AU - Nabaggala, Catherine

AU - John, Chandy C.

AU - Green, Nancy S.

AU - Robberstat, Bjarne

AU - Hensbroek, Boele van

AU - Ter Kuile, Feiko

AU - Phiri, Kamija S.

AU - Opoka, Robert

PY - 2023/11/2

Y1 - 2023/11/2

N2 - Background. Few large prospective studies have evaluated burden and outcomes of malaria in children with sickle cell anaemia (SCA) in malaria endemic countries. We evaluated the incidence, complications and outcome of malaria in three cohorts of Ugandan children with SCA in three areas with differing malaria transmission.Methods. Cohort 1 were SCA aged 3-9 years, enrolled in the hydroxyurea therapy for neurological and cognitive protection in Uganda (BRAINSAFE II) trial at Mulago Hospital, a low transmission area, while cohort 2 and 3 aged 6 months to 15 years, were enrolled in the dihydroartemisinin-piperaquine (DP) or sulphadoxine-pyrimethamine (SP) for the chemoprevention of malaria in SCA (CHEMCHA) trial at Jinja Hospital (moderate transmission) and Kitgum Hospital (high transmission). In cohort 1, all received SP for malaria chemoprophylaxis and hydroxyurea at 20-30mg/kg/day, while cohorts 2 and 3, received either DP or SP for malaria chemoprevention, and a proportion (10%) received hydroxyurea in the study.Results. A total of 706 participants were enrolled: 267, 249 and 190 at Mulago, Jinja and Kitgum respectively. The mean age was 6.5 (SD 3.4) years; 5.1 (1.7), 7.9 (4.3) and 6.8 (3.5) years for Mulago, Jinja, and Kitgum respectively. Incidence of malaria was 13 (95% CI 6, 20) per 100 child years in low, 38 (95% CI 26, 51) in moderate and 104 (95% CI 64, 144) in the high transmission area, p<0.001. Adjusting for hydroxyurea treatment, incidence of malaria was 33 (95%CI 14, 52) per 100 child year on hydroxyurea and 51 (95%CI 40, 62) per 100 child years without hydroxyurea, p=0.001. The most common SCA-related complications were anaemia (39.6%, 133/336), and pain (27.7%, 93/336) among children with malaria. Over a period of 1042.8 person years, there were 115 admissions for malaria, with an overall incidence of 11 per 100 child year (95% CI 9, 13), and this differed across sites, p<0.001. Overall, 1.5% (11/706) children died, and 18.2% (2/11) deaths were directly related to malaria infection.Conclusion. Malaria incidence remains high among Ugandan children with SCA, and differs by transmission patterns. Prevention strategies should be strengthened, especially in high transmission areas.

AB - Background. Few large prospective studies have evaluated burden and outcomes of malaria in children with sickle cell anaemia (SCA) in malaria endemic countries. We evaluated the incidence, complications and outcome of malaria in three cohorts of Ugandan children with SCA in three areas with differing malaria transmission.Methods. Cohort 1 were SCA aged 3-9 years, enrolled in the hydroxyurea therapy for neurological and cognitive protection in Uganda (BRAINSAFE II) trial at Mulago Hospital, a low transmission area, while cohort 2 and 3 aged 6 months to 15 years, were enrolled in the dihydroartemisinin-piperaquine (DP) or sulphadoxine-pyrimethamine (SP) for the chemoprevention of malaria in SCA (CHEMCHA) trial at Jinja Hospital (moderate transmission) and Kitgum Hospital (high transmission). In cohort 1, all received SP for malaria chemoprophylaxis and hydroxyurea at 20-30mg/kg/day, while cohorts 2 and 3, received either DP or SP for malaria chemoprevention, and a proportion (10%) received hydroxyurea in the study.Results. A total of 706 participants were enrolled: 267, 249 and 190 at Mulago, Jinja and Kitgum respectively. The mean age was 6.5 (SD 3.4) years; 5.1 (1.7), 7.9 (4.3) and 6.8 (3.5) years for Mulago, Jinja, and Kitgum respectively. Incidence of malaria was 13 (95% CI 6, 20) per 100 child years in low, 38 (95% CI 26, 51) in moderate and 104 (95% CI 64, 144) in the high transmission area, p<0.001. Adjusting for hydroxyurea treatment, incidence of malaria was 33 (95%CI 14, 52) per 100 child year on hydroxyurea and 51 (95%CI 40, 62) per 100 child years without hydroxyurea, p=0.001. The most common SCA-related complications were anaemia (39.6%, 133/336), and pain (27.7%, 93/336) among children with malaria. Over a period of 1042.8 person years, there were 115 admissions for malaria, with an overall incidence of 11 per 100 child year (95% CI 9, 13), and this differed across sites, p<0.001. Overall, 1.5% (11/706) children died, and 18.2% (2/11) deaths were directly related to malaria infection.Conclusion. Malaria incidence remains high among Ugandan children with SCA, and differs by transmission patterns. Prevention strategies should be strengthened, especially in high transmission areas.

U2 - 10.1182/blood-2023-189066

DO - 10.1182/blood-2023-189066

M3 - Meeting Abstract

SN - 0006-4971

VL - 142

SP - 5327

JO - Blood

JF - Blood

IS - S1

T2 - 65th ASH Annual Meeting

Y2 - 9 December 2023 through 12 December 2023

ER -

Malaria in Children with Sickle Cell Anaemia in Areas with Low, Moderate and High Transmission in Uganda

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