This is a hospital-based, descriptive, cross-sectional study among SCD individuals hospitalized at the Muhimbili National Hospital (MNH). MNH is the national referral hospital in collaboration with Muhimbili University of Health and Allied Sciences, which is the oldest and largest biomedical university in Tanzania. Muhimbili is located in Dar es Salaam on the eastern coast of Tanzania.
The study population consists of individuals with SCD who are already registered in the Muhimbili Sickle Cohort (MSC) and are hospitalized at MNH. The MSC has enrolled 5430 individuals with SCD between 2004 and March 2016. Of these 51.5% and 48.5% are male and female, respectively. The majority (65%) are below the age of 18 years. In this study, we enrolled hospitalized patients who consented and fulfilled inclusion criteria during the 21-monthstudy period (January 2015 to September 2016).
The sample size for this study was estimated to be 369 patients and it was based on the finite population of 800 SCD cases (ie, number of annual SCD hospitalization, from 2014 estimates). This sample has a power of 80% to detect the prevalence of severe anemia of 20% with a 4% margin of error and confidence interval of 95%.
The following inclusion and exclusion criteria were used:
Inclusion criteria
Confirmed SCD; HbSS by High Performance Liquid Chromatography or Hemoglobin Electrophoresis
Enrolled in the MSC
Hospitalization at MNH during the study period
Exclusion criteria
Individuals on hydroxyurea
Blood transfusion in the past 4 weeks
Readmission within the past 4 weeks
The enrolment procedure is illustrated in
Enrolment flow chart. SCD: sickle cell disease.
A general examination was performed that included a record of temperature, weight, blood pressure, peripheral oxygen saturation, pulse, and respiratory rate. Detailed clinical history and physical examination were undertaken to determine the events leading to hospitalization. The study procedures were explained to the patients as well. Details of tests to be performed and samples needed were given to the patients by the study clinician. HIV pretesting counseling was done to all eligible patients. Consent was sought after all the information had been given to the patients.
Confirmed SCD individuals admitted and enrolled were managed according to the standardized guidelines on the management of SCD. Additional investigations were requested depending on clinical indications. Clinical outcomes and laboratory results (
Ten milliliters of blood was collected from all participants under aseptic technique. Of these, 2 mL of blood was collected in a tube with ethylenediamine tetraacetic acid (EDTA) anticoagulant, 2 red tops (serum separator) were filled with 2 mL of blood each, and 4 mL was taken for blood culture. Samples for blood culture were collected in commercially prepared BacTec bottles. In addition, stool and urine samples were collected in empty sterile bottles. All samples were labelled with patients' name, SCD identification number and a special ID number created for the purposes of this study.
Of the EDTA sample, 5µl was used to perform a malaria rapid test (RDT). The remaining sample was used to perform a full blood count. This includes a peripheral blood cell count, both total and differential white cell count, as well as red blood cell indices. These tests were performed immediately after sample collection.
For the serum separated samples, clinical chemistry analysis as well as micronutrient analysis (iron, folate, retinol and B12) were performed on the batched serum samples after enrolment had concluded.
Venous blood in a EDTA tube or capillary blood sample via puncture of a finger was required for the malaria test. The malaria device Pf (HRP2) Ag RDT was used and 5µl of blood was applied to the sample using a pipette or micropipette. 60 µl of assay buffer solution (2 drops of the bottle type) was put into the A well. Results were read in 20 minutes. Correction for white cell count was conducted for counting parasite density in thick films. If the test could not be performed immediately, the blood was stored at 2-8˚C for 3 days. All test components were performed at room temperature.
Quality control was used to assure that the malaria Pf cassette test was working properly and that the results being generated are correct. If no lines were visible, or if no control line (C) formed, whether or not a sample line (T) appeared, the assay was deemed invalid and was repeated with a new sample and cassette.
Thick films for malaria diagnosis was prepared from the blood sample at the time of collection or from the EDTA bottle in the laboratory.
Outcome variable: hemoglobin levels (categorical: Hb <5 g/dL or ≥5 g/dL)
Independent variables
Sociodemographic characteristics
Ethnicity
Residency
Age as continuous and as categorical variable (<18 or ≥18 years)
Sex (categorical: male or female)
Symptoms and signs
Pallor (categorical: Yes [Y] or No [N])
Jaundice (categorical: Y/N), if yes (categorical: tinge, moderate, severe)
O2 saturation-continuous, hypoxia (categorical: <95% or ≥95%)
Enlarged spleen (categorical: Y/N), size (continuous)
Enlarged liver (categorical: Y/N), size (continuous)
Past medical history
Admissions in the past 12 months (categorical: Y/N), frequency (numerical)
Blood transfusion in the past 12 months (categorical: Y/N), frequency (continuous), units (continuous)
Pain in the past 12 months (categorical: Y/N), frequency (continuous)
Stroke in the past 12 months (categorical: Y/N)
History of heart failure (categorical: Y/N)
Laboratory variables (continuous and categorical); see
Hematological: full blood count and reticulocyte count
Parasitology: malaria and hookworm
Microbiology: bacteraemia and HIV infection
Biochemistry: liver and renal function tests, lactate dehydrogenase, C reactive protein, serum folate, vitamin B12, vitamin A and serum iron studies
Thick films were stained using Giemsa staining and examined by microscopy for the presence of malaria parasites using standard methods. The number of parasites (trophozoites) was counted against 200 white blood cells. A slide was reported negative for malaria parasites after at least 100 high-powered microscopic fields were examined. Counting malaria parasites against 200 white blood cells may have resulted in underestimating malaria density as the white cell count in SCD patients tends to be higher due to inflammation and hematology analyzers counting nucleated red blood cells as neutrophils and small lymphocytes. Therefore, ideally, the white cell count should be corrected and “normal” reference values for SCD and non-SCD individuals be calculated and used.
The quality assurance process involved the following: all positive slides were read by a second person. If there were discrepancies between the two readings, then a third person was asked to intervene. For the negative slides, one out of every ten slides was read by a second person
Fresh stool was collected in a clean container to test for hookworm infection. A portion of fresh stool was taken with a spatula or wooden applicator and placed in a test tube, and then the test tube was filled with normal saline. The mixture was mixed well and centrifuged for 5 min at 3000 rpm (Rotina 46, Germany). The supernatant was discarded and with help of a Pasteur pipette, the deposit (stool) was extracted and a small drop was placed on a slide. The deposit on the slide was covered by the cover slip and immediately observed for the hookworm ova under the microscope at 10x magnification. The counting was performed 20 minutes after collection. This method allows for other egg species to be identified
We ensured that samples were collected in a clean container so as to avoid any false positive results. A picture of hookworm ova was available to make sure of correct diagnosis.
The Sysmex XT2000i–Hematology automated analyzer was used to obtain the full blood count. The machine gives a wide range of hematological indices such as white blood cell count, reticulocyte count, hemoglobin levels and platelet count. 2µl of nonclotted venous blood was collected in EDTA tubes (purple caps). The samples were arranged on the roller mixer ready to be tested. Alternatively, the sample was inverted gently end to end (approximately eight times) until the cell bottom of the tube was completely suspended.
On the standard tools bar, the manual section was selected, the patient details were entered and the enter button was pressed. Then the sample vial was held to the needle in front of the start button, and the start button pressed. Once the analysis was done, the results were printed out and reviewed for any panic values, which were then reported to the clinician immediately. If the differential values were missing from the printed results, the sample was diluted in a ratio of 1:5 using the cell pack reagent and the percentage values obtained. After the sample had been analyzed, plasma and buffy coat were obtained and stored under –20°C. This was achieved by centrifuging the EDTA blood at 3000 rpm for 10 minutes, thereafter separating the plasma and buffy coat in graduated cryo-preservative tubes.
The controls for Sysmex machine XT2000i were commercially prepared reagents in 3bottles. Tube one contained low ranges of the hematological indices, tube two for normal and tube three for high hematological values. The quality control procedure was performed before running the samples. The controls needed to be at room temperature before the quality control procedure. The sampler mode from the main menu screen was selected and the tubes were arranged on the sample loader tray with their barcode facing the red barcode light. Then the start button was clicked for the analyzer to start analyzing the controls. Once done, one researcher ensured that the controls had been run on the analyzer and that they were within the acceptable limits.
Architect Kits was used for aspartate aminotransferase (AST), alanine aminotransferase (ALT), creatinine, lactate dehydrogenase (LDH), vitamin B12, folate and C reactive protein (CRP). The Retinol Kit was used for retinol binding protein (vitamin A). The analyzer used was Architect Ci 4100, which includes the chemistry analyzer C4000 (for AST, ALT, creatinine, LDH and CRP2) and the immunoassay analyzer i1000SR (for vitamin B12 and folate). Our samples were stored at –80ºC for a maximum of 90 days.
The batched samples that have been collected throughout the study period will be assayed using a chemistry analyzer (Roche Cobas Mira, New York, USA or Abbott Architect, New York, USA) for the following parameters: bilirubin (total and direct); LDH), iron studies (serum ferritin, serum iron and transferrin saturation), CRP, folate, AST, ALT, vitamin A (retinol) and vitamin B12. Quality assurance was done using commercially prepared reagents that are run on a daily basis with the readings documented following laboratory protocol.
Blood cultures were processed using standard hospital laboratory procedures. Culture media were prepared in a microbiological laboratory and identification followed conventional techniques.
Samples were drawn from patients, stored in the BacTec blood culture bottles, and inserted directly into the instrument as soon as possible to ensure performance efficacy. Before placing vials into the instrument, barcodes were scanned and placed in their assigned stations through the vial entry activity. When scanning barcodes, the vial was placed in the alignment block in front of the scanner with the barcode label facing the scanner. The vial was rotated slightly so that the scanner could read the label. A single beep indicated a successful (good) scan. Station assignments were calculated by the system software to balance the rotor. In order to maintain rotor balance, vials were introduced and placed where the system indicated.
The vial was carefully pushed into the station. In order to ensure that the vial was fully seated in the station, the shoulders were pressed. The vials were not twisted or turned once they were placed in the stations. Vials were not removed except in the following conditions:
Removal of positive
Removal of negative
Identification of anonymous vials
When microorganisms are present, they metabolize nutrients in the culture medium, releasing carbon dioxide, which reacts with a dye in the sensor. The dye modulates the amount of light that is absorbed by a fluorescent material in the sensor. The instrument’s photo detectors then measure the level of fluorescence, which corresponds to the amount of carbon dioxide released by any micro-organisms present. This measurement is interpreted by the system in accordance with the preprogrammed positivity parameters.
Many positive cultures were detected in the first 24 hours after inoculation. Subculturing the positive cultures was done in blood agar, chocolate agar, MacConkey agar, and in other culture media as appropriate. Gram staining was performed for each positive vial. Preliminary antimicrobial susceptibility and identification procedures were performed from fluid in the culture vials.
Ongoing negative vials were kept for 7 days before being discarded as negatives.
Serum/whole blood samples were used for this test. The samples were centrifuged at 3000 rpm for 10 minutes. Thereafter, the serum was graduated 1.25 mL tubes for the HIV test. With whole blood samples, the blood was directly tested for HIV test. The test was performed according to the Tanzania National HIV Rapid Test Algorithm.
All clinical and laboratory information was collected using a preformatted CRF that was designed specifically for this study. This was piloted for a period of 2 weeks and adjusted accordingly. The CRF was reviewed weekly for the first month of data collection to amend variables and improve the quality of data collected. Tools for collecting anthropometric measurements and vital signs were calibrated according to manufacturer’s specifications. All data will be linked to the MSC database, a Web-based system known as MySQL (Sun Microsystems Inc, Santa Clara, California, USA).
Laboratory data is being collected from different sources. For hematology data, the results were printed from hematology analyzers. Results generated from all laboratories were photocopied and the copies were added to the patient’s case notes. The original copies of results were attached to the corresponding CRFs.
Data verification and cleaning is ongoing following double entry, and inconsistencies are being corrected. Missing data, not obtained during the data collection period, will be collected during subsequent visits or by telephone.
The CRFs are stored in filing cabinets and locked, with access only to personnel involved in the study and to a few key personnel who are authorized by the principal investigator. Data backup is done on a daily basis onto 2 storage devices and stored in 2 different physical locations.
Data is double entered and validated in a software application developed using MySQL database and PHP, a server-side HTML scripting language.
Descriptive statistics will be summarized using cross-tabulation and frequencies for categorical data. For continuous variables, measures of central tendencies will be used after checking for normality and transformation where necessary. All estimates will be presented with 95% confidence intervals. Proportions will be compared using Chi-square test of Fisher’s exact test for categorical variables, while continuous variables will be compared using
Modelling procedures will start with the univariate models where the response variable will be fitted against each explanatory variable. Only sets of explanatory variables with a
For univariate and multivariate analyses, it will depend on how the
Baseline laboratory characteristics of the study population.
| Variable | Variable type | Measure of central tendency | Categories |
| Hemoglobin (g/dL) | Numerical, categorical | Mean ± SD | <5, ≥5 |
| Mean corpuscular volume (fl) | Numerical, categorical | Mean ± SD | <80, 80-96, >96 |
| Mean corpuscular hemoglobin (pg) | Numerical, categorical | Mean ± SD | <27, 27-33, >33 |
| Reticulocyte count (%) | Numerical, categorical | Mean ± SD | <0.5, 0.5-1.5, >1.5 |
| White blood count x 10³/L | Categorical | Mean ± SD | ≥11, <11 |
| Malaria | Categorical | Positive, negative | |
| HIV | Categorical | Positive, negative | |
| Stool hookworm | Categorical | Positive, negative | |
| Alanine aminotransferase (U/L) | Numerical, categorical | Mean ± SD | <17, 17-63, >63 |
| Aspartate aminotransferase (U/L) | Numerical, categorical | Mean ± SD | <18, 18-40, >40 |
| Serum creatinine (µmol/L) | Numerical, categorical | Mean ± SD | <62, 62-115, >115 |
| Folate (ng/mL) | Numerical, categorical | Mean ± SD | < 2.6, ≥ 2.6 |
| Retinol (µg/L) | Numerical, categorical | Mean ± SD | <30, 30-80, >80 |
| Vitamin B12 (pg/mL) | Numerical, categorical | Mean ± SD | < 187, ≥187 |
| C reactive protein (mg/L) | Numerical, categorical | Mean ± SD | <8, ≥8 |
| Lactate dehydrogenase (U/L) | Numerical, categorical | Mean ± SD | <50, 50-200, >200 |
| Bacteraemia | Categorical | Yes/no, type, sensitivity | |
| Serum ferritin (ng/mL) | Numerical, categorical | Mean ± SD | <15, 15-200, >200 |
Ethical clearance to conduct the study has been obtained from the Muhimbili University of Health and Allied Sciences and Research and Publication Ethical Committee. A formal written informed consent in Swahili was used for eligible individuals. Nonconsenting patients and those who were not eligible for the study were attended to by the clinical team per SCD management guidelines. Personal, clinical and laboratory information is being kept with utmost confidentiality in keeping with the standards and procedures guiding the organization.