Your search keyword '"Mukaka, Mavuto"' showing total 13 results

1. Pharmacokinetics of single low dose primaquine in Ugandan and Congolese children with falciparum malaria

Author

Mukaka, Mavuto, Onyamboko, Marie A., Olupot-Olupot, Peter, Peerawaranun, Pimnara, Suwannasin, Kanokon, Pagornrat, Watcharee, Kouhathong, Jindarat, Madmanee, Wanassanan, Were, Winifred, Namayanja, Cate, Onyas, Peter, Titin, Harriet, Baseke, Joy, Muhindo, Rita, Kayembe, Daddy K., Ndjowo, Pauline O., Basara, Benjamin B., Bongo, Georgette S., Okalebo, Charles B., Abongo, Grace, Uyoga, Sophie, Williams, Thomas N., Taya, Chiraporn, Dhorda, Mehul, Dondorp, Arjen M., Waithira, Naomi, Imwong, Mallika, Maitland, Kathryn, Fanello, Caterina, Day, Nicholas P.J., Tarning, Joel, White, Nicholas J., and Taylor, Walter R.J.

Published

2023

2. Short intravenous amphotericin B followed by oral posaconazole using a simple, stratified treatment approach for diabetes or COVID-19–associated rhino-orbito-cerebral mucormycosis: author's response.

Author

Mukaka, Mavuto, Manesh, Abi, and Varghese, George M.

Subjects

*AMPHOTERICIN B, *MUCORMYCOSIS, *DIABETES

Published

2023

3. HIV coinfection influences the inflammatory response but not the outcome of cerebral malaria in Malawian children.

Author

Mbale, Emmie W., Moxon, Christopher A., Mukaka, Mavuto, Chagomerana, Maganizo, Glover, Simon, Chisala, Ngawina, Omar, Sofia, Molyneux, Malcolm, Seydel, Karl, Craig, Alister G., Taylor, Terrie, Heyderman, Robert S., and Mallewa, Macpherson

Subjects

MALARIA treatment, HIV infection complications, ANTIGENS, HIV infections, INTERLEUKINS, MALARIA, RESEARCH funding, TUMOR necrosis factors, RETROSPECTIVE studies, DISEASE progression, MIXED infections, DISEASE complications

Abstract

Objectives: Study of the effect of HIV on disease progression in heterogeneous severe malaria syndromes with imprecise diagnostic criteria has led to varying results. Characteristic retinopathy refines cerebral malaria (CM) diagnosis, enabling more precise exploration of the hypothesis that HIV decreases the cytokine response in CM, leading to higher parasite density and a poor outcome.Methods: We retrospectively reviewed data on clinical progression and laboratory parameters in 877 retinopathy-positive CM cases admitted 1996-2011 (14.4% HIV-infected) to a large hospital in Malawi. Admission plasma levels of TNF, interleukin-10, and soluble intercellular adhesion molecule (sICAM-1) were measured by ELISA in 135 retinopathy-positive CM cases.Results: HIV-infected CM cases had lower median plasma levels of TNF (p = 0.008), interleukin-10 (p = 0.045) and sICAM-1 (p = 0.04) than HIV-uninfected cases. Although HIV-infected children were older and more likely to have co-morbidities, HIV-status did not significantly affect parasite density (p = 0.90) or outcome (24.8% infected, vs. 18.5% uninfected; p = 0.13).Conclusion: In this well-characterised CM cohort, HIV-coinfection was associated with marked blunting of the inflammatory response but did not affect parasite density or outcome. These data highlight the complex influence of HIV on severe malaria and bring into question systemic inflammation as a primary driver of pathogenesis in human CM. [ABSTRACT FROM AUTHOR]

Published

2016

4. Sepsis carries a high mortality among hospitalised adults in Malawi in the era of antiretroviral therapy scale-up: A longitudinal cohort study.

Author

Waitt, Peter I., Mukaka, Mavuto, Goodson, Patrick, SimuKonda, Felanji D., Waitt, Catriona J., Feasey, Nick, Allain, Theresa J., Downie, Paul, and Heyderman, Robert S.

Abstract

Summary Objective To assess mortality risk among adults presenting to an African teaching hospital with sepsis and severe sepsis in a setting of high HIV prevalence and widespread ART uptake. Methods Prospective cohort study of adults (age ≥16 years) admitted with clinical suspicion of severe infection between November 2008 and January 2009 to Queen Elizabeth Central Hospital, a 1250-bed government-funded hospital in Blantyre, Malawi. Demographic, clinical and laboratory information, including blood and cerebrospinal fluid cultures were obtained on admission. Results Data from 213 patients (181 with sepsis and 32 with severe sepsis; M:F = 2:3) were analysed. 161 (75.6%) patients were HIV-positive. Overall mortality was 22%, rising to 50% amongst patients with severe sepsis. The mortality of all sepsis patients commenced on antiretroviral therapy (ART) within 90 days was 11/28 (39.3%) compared with 7/42 (16.7%) among all sepsis patients on ART for greater than 90 days ( p = 0.050). Independent associations with death were hypoxia (OR = 2.4; 95% CI, 1.1–5.1) and systolic hypotension (OR 7.0; 95% CI: 2.4–20.4). Conclusions Sepsis and severe sepsis carry high mortality among hospitalised adults in Malawi. Measures to reduce this, including early identification and targeted intervention in high-risk patients, especially HIV-positive individuals recently commenced on ART, are urgently required. [ABSTRACT FROM AUTHOR]

Published

2015

5. Genomic pneumococcal load and CSF cytokines are not related to outcome in Malawian adults with meningitis.

Author

Wall, Emma C., Gritzfeld, Jenna F., Scarborough, Matthew, Ajdukiewicz, Katherine M.B., Mukaka, Mavuto, Corless, Caroline, Lalloo, David G., and Gordon, Stephen B.

Abstract

Summary Objective Bacterial meningitis in sub-Saharan Africa is predominantly caused by Streptococcus pneumoniae , is often associated with HIV co-infection and mortality rates are double those seen in better resourced settings. Methods To investigate the cause of this excessive mortality we quantified the pneumococcal DNA load and six common pro-inflammatory cytokines in the cerebrospinal fluid (CSF) of Malawian adults with culture proven pneumococcal meningitis and correlated the results to clinical parameters and outcome. There are currently no published data relating bacterial load to outcome in adults with pneumococcal meningitis. Results The mean age of patients was 32 years, 82% were HIV infected and 49% had died by day 40. CSF bacterial loads were high (median 6.5 × 10 5 copies/ml CSF) and there was no significant variation in bacterial load between survivors and non-survivors. All pro-inflammatory CSF cytokines were elevated in the CSF, with no clinically important differences between survivors and non-survivors. HIV status did not affect the CSF bacterial load or cytokine response. Conclusion Mortality from pneumococcal meningitis in adults in sub-Saharan Africa is not related to pneumococcal bacterial load. More research is needed to understand the very high mortality from meningitis in this region. [ABSTRACT FROM AUTHOR]

Published

2014

6. Short intravenous amphotericin B followed by oral posaconazole using a simple, stratified treatment approach for diabetes or COVID-19-associated rhino-orbito-cerebral mucormycosis: a prospective cohort study.

Author

Manesh, Abi, Devasagayam, Emily, Bhanuprasad, Kundakarla, Varghese, Lalee, Kurien, Regi, Cherian, Lisa M., Dayanand, Divya, George, Mithun M., Kumar, Selwyn S., Karthik, Rajiv, Vanjare, Harshad, Peter, Jayanthi, Michael, Joy S., Thomas, Meera, Mathew, Binu S., Samuel, Prasanna, Peerawaranun, Pimnara, Mukaka, Mavuto, Rupa, Vedantam, and Varghese, George M.

Subjects

*AMPHOTERICIN B, *DIABETIC acidosis, *MUCORMYCOSIS, *GLYCEMIC control, *INTRAVENOUS therapy, *COHORT analysis

Abstract

To evaluate the efficacy and safety of short-course intravenous amphotericin B followed by sustained release posaconazole tablets for diabetes or COVID-19-associated rhino-orbito-cerebral mucormycosis. This prospective, pragmatic study included adults with diabetes or COVID-19-associated rhino-orbito-cerebral mucormycosis. Patients received short (7–14 days) or long (15–28 days) intravenous antifungal therapy (short intravenous antifungal treatment [SHIFT] or long intravenous antifungal treatment [LIFT], respectively) depending on the presence or absence of brain involvement. All patients received step-down posaconazole tablets, debridement, and glycemic control. The primary outcome was the treatment success at week 14, which was determined by assessing survival and the absence of disease progression through clinical evaluation and nasal endoscopy. Log-binomial regression analysis (risk ratio and 95% CI) was performed to assess factors associated with the primary outcome. Intravenous therapy was administered to 251 participants: SHIFT, 205 (median duration, 13 days); LIFT, 46 (median duration, 22 days). Treatment success at 3 months was 88% (217/248; 95% CI, 83–91%): SHIFT group, 93% (189/203; 89–96%); LIFT group, 62% (28/45; 47–76%). All-cause mortality was 12% (30/251): SHIFT group, 6% (13/205); LIFT group, 37% (17/46). Age (aRR [95% CI]: 1.02 [1.00–1.05]; p 0.027), diabetic ketoacidosis at presentation (2.32 [1.20–4.46]; p 0·012), glycated haemoglobin A1c (1.19 [1.03–1.39]; p 0.019), stroke (3.93 [1.94–7.95]; p 0·0001), and brain involvement (5.67 [3.05–10.54]; p < 0.0001) were independently associated with unsuccessful outcomes. : Short intravenous amphotericin B with step-down posaconazole tablets should be further studied as primary treatment option for diabetes or COVID-19-associated mucormycosis in randomized controlled trials. [ABSTRACT FROM AUTHOR]

Published

2023

7. Sepsis: Markers of Mortailty in Malawi.

Author

Waitt, Peter, Downie, Paul, Mukaka, Mavuto, Toh, Chen Hok, and Heyderman, Robert

Published

2009

8. Community seroprevalence and risk factors for SARS-CoV-2 infection in different subpopulations in Vellore, India, and their implications for future prevention.

Author

Dayanand, Divya, Irudhayanathan, Indhuja, Kundu, Debasree, Manesh, Abi, Abraham, Vinod, Abhilash, Kundavaram PP, Chacko, Binila, Moorthy, Mahesh, Samuel, Prasanna, Peerawaranun, Pimnara, Mukaka, Mavuto, Joseph, Jayaraj, Sivaprakasam, Mohanasankar, and Varghese, George M

Subjects

*SEROPREVALENCE, *SARS-CoV-2, *CORONAVIRUS diseases, *HEALTH policy, *HIV seroconversion, *VACCINATION status, *RURAL population

Abstract

• The seroprevalence of SARS-CoV-2 in Vellore, India had reached over 70% by July 2021 • Seroprevalence varied according to subpopulation, with the highest levels found in urban slums • The vast majority of the infections (75%) were asymptomatic • Vaccine uptake among urban slums and the rural population was poor • A targeted vaccination for high-risk individuals is suggested The aim of this study was to inform public health policy decisions through the assessment of IgG antibody seroprevalence in the population and the risk factors for SARS-CoV-2 infection. The seroprevalence of IgG antibodies among different subpopulations at the end of the first and second waves of the pandemic was estimated. Various risk factors associated with seropositivity, including sociodemography, IgG antibodies against endemic human coronavirus, and vaccination status, were also assessed. For all 2433 consenting participants, the overall estimated seroprevalences at the end of first and second waves were 28.5% (95% CI 22.3–33.7%) and 71.5% (95% CI 62.8–80.5%), respectively. The accrual of IgG positivity was heterogeneous, with the highest seroprevalences found in urban slum populations (75.1%). Vaccine uptake varied among the subpopulations, with low rates (< 10%) among rural and urban slum residents. The majority of seropositive individuals (75%) were asymptomatic. Residence in urban slums (OR 2.02, 95% CI 1.57–2.6; p < 0.001), middle socioeconomic status (OR 1.77, 95% CI 1.17–2.67; p = 0.007), presence of diabetes (OR 1.721, 95% CI 1.148–2.581; p = 0.009), and hypertension (OR 1.75, 95% CI 1.16–2.64; p = 0.008) were associated with seropositivity in multivariable analyses. Although considerable population immunity has been reached, with more than two-thirds seropositive, improved vaccination strategies among unreached subpopulations and high-risk individuals are suggested for better preparedness in future. [ABSTRACT FROM AUTHOR]

Published

2022

9. Parasites bearing a single copy of the multi-drug resistance gene (pfmdr-1) with wild-type SNPs predominate amongst Plasmodium falciparum isolates from Malawi

Author

Nkhoma, Standwell, Nair, Shalini, Mukaka, Mavuto, Molyneux, Malcolm E., Ward, Stephen A., and Anderson, Timothy J.C.

Subjects

*ANTIMALARIALS, *QUINOLINE, *INFECTION

Abstract

Abstract: We genotyped 160 P. falciparum infections from Malawi for pfmdr-1 copy number changes and SNPs associated with in vivo tolerance and poor in vitro sensitivity to the component drugs of Coartem. We also measured in vitro susceptibility of 49 of these isolates to a variety of drugs in clinical use or with a potential for use in Africa. All 160 infections carried a single copy of pfmdr-1 but 34% exhibited sequence variation at 4 of the 5 polymorphic sites in pfmdr-1. Isolates carrying 86-Asn and 184-Tyr pfmdr-1 alleles were significantly less sensitive (p <0.001) to mefloquine, lumefantrine, artemether and dihydroartemisinin compared with those bearing 86-Tyr and 184-Phe polymorphisms. This study provides baseline measures prior to policy change: continued surveillance for changes in baseline drug susceptibility, pfmdr-1 copy number and SNPs, and other putative Coartem resistance loci will be necessary to provide an early warning of emerging Coartem resistance in this setting. [Copyright &y& Elsevier]

Published

2009

10. Arterolane–piperaquine–mefloquine versus arterolane–piperaquine and artemether–lumefantrine in the treatment of uncomplicated Plasmodium falciparum malaria in Kenyan children: a single-centre, open-label, randomised, non-inferiority trial

Author

Hamaluba, Mainga, van der Pluijm, Rob W, Weya, Joseph, Njuguna, Patricia, Ngama, Mwanajuma, Kalume, Peter, Mwambingu, Gabriel, Ngetsa, Caroline, Wambua, Juliana, Boga, Mwanamvua, Mturi, Neema, Lal, Altaf A, Khuroo, Arshad, Taylor, Walter R J, Gonçalves, Sónia, Miotto, Olivo, Dhorda, Mehul, Mutinda, Brian, Mukaka, Mavuto, and Waithira, Naomi

Subjects

*DRUG therapy for malaria, *PROTOZOA physiology, *QUINOLINE, *PROTOZOA, *RESEARCH, *HETEROCYCLIC compounds, *ORAL drug administration, *RESEARCH methodology, *MEFLOQUINE, *MEDICAL cooperation, *EVALUATION research, *HYDROCARBONS, *PEROXIDES, *TREATMENT effectiveness, *COMPARATIVE studies, *RESEARCH funding, *ANTIMALARIALS

Abstract

Background: Triple antimalarial combination therapies combine potent and rapidly cleared artemisinins or related synthetic ozonides, such as arterolane, with two, more slowly eliminated partner drugs to reduce the risk of resistance. We aimed to assess the safety, tolerability, and efficacy of arterolane-piperaquine-mefloquine versus arterolane-piperaquine and artemether-lumefantrine for the treatment of uncomplicated falciparum malaria in Kenyan children.Methods: In this single-centre, open-label, randomised, non-inferiority trial done in Kilifi County Hospital, Kilifi, coastal Kenya, children with uncomplicated Plasmodium falciparum malaria were recruited. Eligible patients were aged 2-12 years and had an asexual parasitaemia of 5000-250 000 parasites per μL. The exclusion criteria included the presence of an acute illness other than malaria, the inability to tolerate oral medications, treatment with an artemisinin derivative in the previous 7 days, a known hypersensitivity or contraindication to any of the study drugs, and a QT interval corrected for heart rate (QTc interval) longer than 450 ms. Patients were randomly assigned (1:1:1), by use of blocks of six, nine, and 12, and opaque, sealed, and sequentially numbered envelopes, to receive either arterolane-piperaquine, arterolane-piperaquine-mefloquine, or artemether-lumefantrine. Laboratory staff, but not the patients, the patients' parents or caregivers, clinical or medical officers, nurses, or trial statistician, were masked to the intervention groups. For 3 days, oral artemether-lumefantrine was administered twice daily (target dose 5-24 mg/kg of bodyweight of artemether and 29-144 mg/kg of bodyweight of lumefantrine), and oral arterolane-piperaquine (arterolane dose 4 mg/kg of bodyweight; piperaquine dose 20 mg/kg of bodyweight) and oral arterolane-piperaquine-mefloquine (mefloquine dose 8 mg/kg of bodyweight) were administered once daily. All patients received 0·25 mg/kg of bodyweight of oral primaquine at hour 24. All patients were admitted to Kilifi County Hospital for at least 3 consecutive days and followed up at day 7 and, thereafter, weekly for up to 42 days. The primary endpoint was 42-day PCR-corrected efficacy, defined as the absence of treatment failure in the first 42 days post-treatment, of arterolane-piperaquine-mefloquine versus artemether-lumefantrine, and, along with safety, was analysed in the intention-to-treat population, which comprised all patients who received at least one dose of a study drug. The 42-day PCR-corrected efficacy of arterolane-piperaquine-mefloquine versus arterolane-piperaquine was an important secondary endpoint and was also analysed in the intention-to-treat population. The non-inferiority margin for the risk difference between treatments was -7%. The study is registered in ClinicalTrials.gov, NCT03452475, and is completed.Findings: Between March 7, 2018, and May 2, 2019, 533 children with P falciparum were screened, of whom 217 were randomly assigned to receive either arterolane-piperaquine (n=73), arterolane-piperaquine-mefloquine (n=72), or artemether-lumefantrine (n=72) and comprised the intention-to-treat population. The 42-day PCR-corrected efficacy after treatment with arterolane-piperaquine-mefloquine (100%, 95% CI 95-100; 72/72) was non-inferior to that after treatment with artemether-lumefantrine (96%, 95% CI 88-99; 69/72; risk difference 4%, 95% CI 0-9; p=0·25). The 42-day PCR-corrected efficacy of arterolane-piperaquine-mefloquine was non-inferior to that of arterolane-piperaquine (100%, 95% CI 95-100; 73/73; risk difference 0%). Vomiting rates in the first hour post-drug administration were significantly higher in patients treated with arterolane-piperaquine (5%, 95% CI 2-9; ten of 203 drug administrations; p=0·0013) or arterolane-piperaquine-mefloquine (5%, 3-9; 11 of 209 drug administrations; p=0·0006) than in patients treated with artemether-lumefantrine (1%, 0-2; three of 415 drug administrations). Upper respiratory tract complaints (n=26 for artemether-lumefantrine; n=19 for arterolane-piperaquine-mefloquine; n=23 for arterolane-piperaquine), headache (n=13; n=4; n=5), and abdominal pain (n=7; n=5; n=5) were the most frequently reported adverse events. There were no deaths.Interpretation: This study shows that arterolane-piperaquine-mefloquine is an efficacious and safe treatment for uncomplicated falciparum malaria in children and could potentially be used to prevent or delay the emergence of antimalarial resistance.Funding: UK Department for International Development, The Wellcome Trust, The Bill & Melinda Gates Foundation, Sun Pharmaceutical Industries. [ABSTRACT FROM AUTHOR]

Published

2021

11. The persistence and oscillations of submicroscopic Plasmodium falciparum and Plasmodium vivax infections over time in Vietnam: an open cohort study.

Author

Nguyen, Thuy-Nhien, von Seidlein, Lorenz, Nguyen, Tuong-Vy, Truong, Phuc-Nhi, Hung, Son Do, Pham, Huong-Thu, Nguyen, Tam-Uyen, Le, Thanh Dong, Dao, Van Hue, Mukaka, Mavuto, Day, Nicholas PJ, White, Nicholas J, Dondorp, Arjen M, Thwaites, Guy E, and Hien, Tran Tinh

Subjects

*BACTERIAL diseases, *PLASMODIUM falciparum, *PLASMODIUM vivax, *PUBLIC health, *INFECTIOUS disease transmission, MALARIA transmission

Abstract

Summary Background A substantial proportion of Plasmodium species infections are asymptomatic with densities too low to be detectable with standard diagnostic techniques. The importance of such asymptomatic plasmodium infections in malaria transmission is probably related to their duration and density. To explore the duration of asymptomatic plasmodium infections and changes in parasite densities over time, a cohort of participants who were infected with Plasmodium parasites was observed over a 2-year follow-up period. Methods In this open cohort study, inhabitants of four villages in Vietnam were invited to participate in baseline and subsequent 3-monthly surveys up to 24 months, which included the collection of venous blood samples. Samples were batch-screened using ultra-sensitive (u)PCR (lower limit of detection of 22 parasites per mL). Participants found to be infected by uPCR during any of these surveys were invited to join a prospective cohort and provide monthly blood samples. We estimated the persistence of Plasmodium falciparum and Plasmodium vivax infections and changes in parasite densities over a study period of 24 months. Findings Between Dec 1, 2013, and Jan 8, 2016, 356 villagers participated in between one and 22 surveys. These study participants underwent 4248 uPCR evaluations (11·9 tests per participant). 1874 (32%) of 4248 uPCR tests indicated a plasmodium infection; 679 (36%) of 1874 tests were P falciparum monoinfections, 507 (27%) were P vivax monoinfections, 463 (25%) were co-infections with P falciparum and P vivax , and 225 (12%) were indeterminate species of Plasmodium . The median duration of P falciparum infection was 2 months (IQR 1–3); after accounting for censoring, participants had a 20% chance of having parasitaemia for 4 months or longer. The median duration of P vivax infection was 6 months (3–9), and participants had a 59% chance of having parasitaemia for 4 months or longer. The parasite densities of persistent infections oscillated; following ultralow-density infections, high-density infections developed frequently. Interpretation Persistent largely asymptomatic P vivax and P falciparum infections are common in this area of low seasonal malaria transmission. Infections with low-density parasitaemias can develop into much higher density infections at a later time, which are likely to sustain malaria endemicity. Funding The Wellcome Trust, Bill & Melinda Gates Foundation. [ABSTRACT FROM AUTHOR]

Published

2018

12. Subtle changes in Plasmodium falciparum infection complexity following enhanced intervention in Malawi.

Author

Sisya, Tamika J., Kamn’gona, Raphael M., Vareta, Jimmy A., Fulakeza, Joseph M., Mukaka, Mavuto F.J., Seydel, Karl B., Laufer, Miriam K., Taylor, Terrie E., and Nkhoma, Standwell C.

Subjects

*PLASMODIUM falciparum, *MALARIA prevention, *ARTEMISININ, *MALARIA diagnosis, *BIOLOGICAL variation, *THERAPEUTICS

Abstract

With support from the Global Fund, the United States President's Malaria Initiative (PMI) and other cooperating partners, Malawi is implementing a comprehensive malaria control programme involving indoor residual spraying in targeted districts, universal coverage with insecticide-treated bed nets, use of rapid diagnostic tests to confirm the clinical diagnosis of malaria and use of the highly effective artemisinin-based combination therapy, artemether-lumefantrine (AL), as the first-line treatment for malaria. We genotyped 24 genome-wide single nucleotide polymorphisms (SNPs) in Plasmodium falciparum infections ( n = 316) sampled from a single location in Malawi before (2006 and 2007) and after enhanced intervention (2008 and 2012). The SNP data generated were used to examine temporal changes in the proportion of multiple-genotype infections (MIs), mean number of heterozygous SNPs within MIs, parasite genetic diversity (expected heterozygosity and genotypic richness), multilocus linkage disequilibrium and effective population size ( N e ). While the proportion of MIs, expected heterozygosity, genotypic richness, multilocus linkage disequilibrium and N e were unchanged over time, the mean number (±standard deviation) of heterozygous SNPs within MIs decreased significantly ( p = 0.01) from 9(±1) in 2006 to 7(±1) in 2012. These findings indicate that the genetic diversity of P. falciparum malaria parasites in this area remains high, suggesting that only subtle gains, if any, have been made in reducing malaria transmission. Continued surveillance is required to evaluate the impact of malaria control interventions in this area and the rest of Malawi, and to better target control interventions. [ABSTRACT FROM AUTHOR]

Published

2015

13. Kaposi’s sarcoma in children: An open randomised trial of vincristine, oral etoposide and a combination of vincristine and bleomycin.

Author

Chagaluka, George, Stanley, Christopher, Banda, Kondwani, Depani, Sarita, Nijram’madzi, Jenala, Katangwe, Thembie, Israels, Trijn, Bailey, Simon, Mukaka, Mavuto, and Molyneux, Elizabeth

Published

2014