Preventing Stroke in Sickle Cell Anaemia Clinical Trial
Official title:
Preventing Stroke Triggers in Children With Sickle Cell Anaemia in Mulago Hospital, Kampala (PREST ): a Randomized Control Trial
Sickle cell anaemia (SCA) is a common hereditary haemoglobin disorder in Africa. World wide
it is estimated that about 300,000 newborns are born every year. Of which 75% of them live in
Sub-saharan Africa (SSA). In Uganda, about 15,000 babies are born with sickle cell disease
per year.
In Uganda, the stroke prevalence was found to be 6.2% in children admitted to the National
referral hospital in Kampala. Notable between 21 to 30% of these children presented with
co-morbidities such as anaemia, bacteraemia and painfull crisis. Stroke in SCA is mediated by
several mechanism such as cellular adhesions, inflammatory markers, hemolysis associated
oxidative stress and hemostatic activation. Stroke in SCA is primarily a large vessel stroke
and the mechanisim state above lead to a narrowing of the lumen of the cerebral arteries
Arterial ischaemic stroke which occurs frequently in children with SCA has been associated
with bacterial infections. Recent studies have shown that minor infections such as flu like
infections can play a critical role in the trigger of stroke in children.
Our hypothesis is that viral flu infections is a key trigger for the risk of stroke in
children with SCA. Our objective is to prevent the occurrence of flu illnesses in children
with SCA thereby reducing the risk for stroke in our population of children with SCA.
Methods: A randomized controlled double blinded study Study site: The study will be conducted
at the Sickle Cell Clinic (SCC), Mulago Hospital. Inclusion criteria: will be ;age between 2
years and 12 years;All children whose parents will have consented and those above 7years will
have to assent. Exclusion criteria: all children with previous strokes; children who have
acute illness and are not clinically stable; any child with previous documented adverse event
following immunization (AEFI).
Sample Size: Using Open EPI calculator for cohort studies we calculated a total sample size
of 136 participant to achieve our objective. Using a 95% confidence interval, power of 80%
and an unexposed outcome of 25% (4) using a ratio of 1:1. Each arm will have 68 participants.
With anticipated 10% loss to follow up a total sample size of 150 with each arm having 75
participants.
Study utility: Globally, stroke triggers have been recently identified independent of the
existing risk factors such as high cerebral velocity speeds on TCDs. Flues like illnesses
have been reported to be stroke triggers in children with arterial ischaemic strokes
worldwide.This study may influence the role of influenza vaccination in the prevention of
stroke triggers in children with sickle cell anaemia. It will also add to the existing
modalities which have helped to reduce the incidence of stroke amongst this high risk group
of children with
Preventing Stroke Triggers in Children with Sickle Cell Anaemia in Mulago Hospital, Kampala
(PREST): A Randomized Control Trial
Principal Investigator: Deogratias Munube ( MBChB, MMed) Department of Paediatrics and Child
Health
Mentor: Prof . James.K. Tumwine (MBChB, MMed, PhD) Prof . Grace Ndeezi (MBChB, MMed, PhD)
Research hypothesis: Our hypothesis is that viral flu infections is a key trigger for the
risk of stroke in children with SCA. Our objective is to prevent the occurrence of flu
illnesses in children with SCA thereby reducing the risk for stroke in our population of
children with SCA.
Rational for research: Globally, stroke triggers have been recently identified independent of
the existing risk factors such as high cerebral velocity speeds on TCDs. Flues like illnesses
have been reported to be stroke triggers in children with arterial ischaemic strokes
worldwide. This study may influence the role of influenza vaccination in the prevention of
stroke triggers in children with sickle cell anaemia. It will also add to the existing
modalities which have helped to reduce the incidence of stroke amongst this high risk group
of children with
Methods: Study design: This will be a randomized controlled double blinded study Study site:
The study will be conducted at the Sickle Cell Clinic (SCC), Mulago Hospital.
Study population: The study will include individuals with Sickle cell anaemia attending the
sickle cell clinic services at Mulago National Referral Hospital.
Inclusion criteria: Age between 2 years and 12 years; all children whose parents will have
consented and those above 7years will have to assent Exclusion criteria: All children with
previous strokes; Children who have acute illness and are not clinically stable; any child
with previous documented adverse event following immunization (AEFI).
Sample Size: Using Open EPI calculator for cohort studies we calculated a total sample size
of 136 participants to achieve our objective. Using a 95% confidence interval, power of 80%
and an unexposed outcome of 25% (4) using a ratio of 1:1. Each arm will have 68 participants.
With anticipated 10% loss to follow up a total sample size of 150 with each arm having 75
participants.
The following will be done to achieve a randomized control trial:
1. Randomization
2. Blinding
3. Study variables:
Primary outcome: Incidence of stroke: The incidence of stroke is defined as the occurrence of
a focal neurological deficit in a child lasting at least 24 hours if it has a vascular basis
during the study period. Each child suspected to have stroke will have a brain cranial
tomography (CT) scan done to confirm the diagnosis. This diagnosis will then be adjudicated
by a team comprising of a pediatrician, neurologist and a radiologist.
Secondary outcomes: The levels of inflammatory markers VCAM-1 and gene profile IL4R 503P
locus: blood will extracted from a participant by veni-puncture every 6 months and whenever a
participant comes to the clinic when ill or is admitted, Acute chest syndrome, Pneumonia.
Trans-cranial Doppler scan speeds: a TCD will be performed for each participant every 6
months and whenever the participant is admitted or comes to the clinic when ill. The speeds
will be noted.
Investigational products: influenza vaccine: An inactivated influenza vaccine (split virion)
shall be used during the study. The product information is attached as an appendix to the
proposal.
Study product acquisition: The product will be acquired from Laborex pharmaceutical, Sure
House, Bombo road, Kampala.The vaccine is an injectable packaged in a vial Preparation,
administration and dosage of the influenza vaccine to be used for the study Placebo: Placebo
will be the sterile water for injection which shall be withdrawn from a vial for each
participant.
Recruitment procedures: All children with SCD from 2 to 12 years presenting at the sickle
cell clinic will be assessed for eligibility by a study nurse. Eligible participant will then
be taken through the consenting process. Participants whose parents have consented and have
themselves assented when appropriate will then be randomized to either the influenza vaccine
or placebo arm.
Schedule of follow up visits: After enrolment, each participant will be given a 6 month
appointment for a review and a subsequent repeat of the TCDs. At the end of the 12 month
follow up, each participant will at closure have repeat TCDs.
Blood investigations: At enrollment, blood will be drawn by venipuncture to assess for the
inflammatory VCAM-1 and gene profile IL4R 503P locus, complete blood count panel, serum
creatinine, serum urea and electrolytes, liver function tests.
Study visits: The study visits will include a baseline visit at enrollment, every 6 months
and whenever the patient comes to the clinic or admitted at the pediatric emergence unit at
Mulago National referral hospital. Patients who miss their scheduled study visits will be
called within a week and actively followed to attend the visit before the month lapses.
Patients who miss two consecutive study visits will be considered lost to follow up and
attempts will be made to establish their current state as to whether they have a stroke.
Adverse effects monitoring: The participants will be counseled to report any untoward effect
that they experience after receiving a study drug following GCP/ICH criteria. An adverse
monitoring form will be completed for each study visit. Serious adverse effects that are
potentially fatal or fatal will be reported to the ethics review board within 24hours of the
occurrence of the adverse effect.
Local safety and data safety and monitoring committee: A data safety and monitoring committee
will be set up to review the data so as to ascertain the continuous safety of the study
drugs. This committee will comprise of a senior consultant pediatrician, biostatician and
research scientist.
Stopping rules: There shall be no stopping rules Data Management: The principal investigator,
co-investigator and clinical research nurses will have access to records.
Quality control and quality assurance: Data will be evaluated for compliance with protocol
and accuracy in relation to source documents. The study will be conducted in accordance with
procedures identified in the protocol. SOPs will be used at all clinical and laboratory
sites.
Ethics/protection of human subjects: This protocol will be approved by Makerere University
College of Health Sciences School of Medicine Research and Ethics Committee and the Uganda
National Council of Science and Technology before this study commences. Consent shall be got
from the parents and assent will be sought from the children above 8.
Informed Consent Process: Written informed consent will be obtained from the parents and
assent sought from the children above 8 years of aged.. Parents will be provided with
literature on the symptoms and signs of stroke in order to enable them return to the
hospital.
Subject Confidentiality: All records will be kept in a locked filing cabinet, which is
accessed only by the investigators and the study nurse(s). All computer entry and networking
programs will be done with coded numbers and initials only. Only the investigators, the
clinical monitor, the ethics committees or any other regulatory agencies, at the request of
the collaborator will have access to the records. Every effort will be taken to maintain
confidentiality.
The study protocol, documentation, data and all other information generated will be held in
strict confidence. Clinical information will not be released without written permission of
the parents, except as necessary for monitoring. No information concerning the study or the
data will be released to any unauthorized third party, without prior written approval of the
sponsor.
Data handling and record keeping The Principal Investigator will be the data manager with
responsibility for receiving, entering, cleaning, querying, analysing and storing all data
that accrues from the study. He will be responsible for linking the epidemiological and
clinical data from the field and the clinic with the laboratory data from the immunology,
haematology and genetics laboratories.
Study Records Retention: Essential documents will be retained until at least 2 years after
the last approval of a marketing application in an ICH region and until there are no pending
or contemplated marketing applications in an ICH region or at least 2 years have elapsed
since the formal discontinuation of clinical development of the investigational product.
These documents will be retained for a longer period however if required by the applicable
regulatory requirements or by an agreement with the sponsor. It is the responsibility of the
sponsor to inform the investigator/institution as to when these documents no longer need to
be retained
Protocol Deviations:The investigator will conduct the trial in compliance with the protocol
agreed to by the sponsor and the regulatory authority and which was given approval by ethics.
The investigator will sign the protocol to confirm agreement. In event of a deviation all
relevant authorities will be informed.
Data analysis: Data will be entered using EPI info version 6.0.The primary end point will be
the incidence of stroke at 12 month follow up. The incidence will be calculated as the number
of new cases that have occurred during the given interval of time divided by the population
at risk at the beginning of the time interval. Data will be analyzed using SPSS version 16
(SPSS Inc, Chicago, IL, USA). Both uni-variate analysis and bi-variate analysis will be done.
The primary analyses will be performed with an intention to treat with p <0.05 considered
significant. . Survival analysis will be used to compare between the two groups. In order to
assess for time to event, we shall construct Kaplan Meier survival curves. The outcomes will
be compared using a log rank test to determine if differences are statistically significant.
The relative risks will be calculated as the measures of association as well as absolute
difference in the outcomes. Missing data will be recorded as missing and not analyse.
Conflict of interest: None
Collaborative agreements: None
Intended use of results:
Study findings will upon completion of the study be compiled into a report that will be
copied or made available to the following: Nurture program, department of paediatrics and
child health, Sir Albert cook library, the Sickle Cell Clinic, Ministry of Health. Findings
will be presented in both local and international conferences. Manuscripts will also be
prepared for publication in peer reviewed scientific journals.
Other information: The trial is not supported by another grant.
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