High Blood Pressure Clinical Trial
Official title:
Pilot Evaluation of the Effect of Riboflavin Supplementation on Blood Pressure and Possible Effect Modification by the MTHFR C677T Genotype
Hypertension, which results from a combination of multiple lifestyle and genetic factors, is
a global public health problem affecting 1 billion people worldwide. The identification of
cheap treatment interventions without adverse side effects would be hugely advantageous
particularly in low-income settings with high prevalence of hypertension such as sub-Saharan
Africa where up to 46% of adults are affected.
Emerging evidence links a functional polymorphism in the MTHFR gene (rs1801133 C677T),
encoding the folate-metabolising enzyme methylenetetrahydrofolate reductase to high blood
pressure in adults. Variation at rs1801133 is relatively common and has 3 genotypes;
homozygous "normal" CC, heterozygous CT and homozygous "variant" TT genotypes. Of these
genotypes, the homozygous "variant" TT is more strongly associated with a higher BP. The
precise mechanism by which MTHFR is associated with BP remains unclear. It has been recently
shown in 3 separate randomized controlled trials that BP is highly responsive to riboflavin
and that this response is differential by MTHFR rs1801133 genotype. In all these clinical
trials, significant reduction in both systolic and diastolic blood pressure was observed in
the homozygous variant TT genotype and an intermediate effect seen in those with the
heterozygous CT genotype. The aim of this study is to evaluate the effect of riboflavin
supplementation on blood pressure in a riboflavin-deplete population as well as comparing
plasma riboflavin status before and after supplementation. This will be achieved by
conducting a randomized single-blind placebo controlled trial over a period of 16 weeks.
The Investigators will use the Keneba biobank to invite about 100 adults with the CT genotype
and a similar number of age-, sex and village-matched CC homozygotes. Participants within
each of the groups will be randomized to receive either riboflavin (5mg/d) or a matching
placebo which would be supplied on a weekly basis. Blood sample, blood pressure measurement,
socio-demographic data and their anthropometric measurements (height, weight, waist and hip
circumference and body composition by BIA) will be taken during the initial visit. An
additional blood sample will be taken at the end of the study whilst additional BP
measurements will be taken respectively at 8 weeks and at the end of the intervention. The
possibility that riboflavin deficiency represents a new, easily-correctible causal factor in
hypertension in sub-Saharan Africa would require further large-scale interventions if this
pilot study yields encouraging results.
This is a recall-by-genotype randomized single-blind placebo-controlled micronutrient
supplementation trial. The Keneba biobank will be used to identify all potential participants
i.e. individuals genotyped for MTHFR C677T for this pilot study.
The Investigators will invite all 163 adults with the CT genotype in the Keneba biobank and a
similar number of age- sex- and village-matched CC homozygotes to participate in the study.
Field assistants will visit the homes of potentially eligible participants, to provide full
information about the purpose and methods of the study, potential risks and benefits, and
participants' rights. Participants will then provide written informed consent. The field
assistant will ensure that the conversation and consent process occurs in a private area or
room, to maintain privacy and confidentiality. After exclusions and non-consenters the
investigators anticipate at least 102 subjects per group. Using standard deviation estimates
from our own and published literature (14mmHg for SBP and 10mmHg for DBP) the investigators
will have 95% confidence (at p<0.05) of detecting differences of 3.88mmHg for SBP and
2.76mmHg for DBP.
Participants within each of the groups will be randomized to riboflavin or placebo in a 1:1
ratio according to a computer generated randomization scheme. This will be done by randomly
assigning study numbers within the CT carriers to a treatment group and enrolling
participants sequentially from lowest to highest study identification number. The subjects
will be randomized upon dispensing the study drug associated with the subject pair's study
identification number. Field, clinical, laboratory and data entry staff will be blinded to
the genotype of the study participants and to the identity of the treatment arm to which a
participant is assigned from the time of randomization to the time of unblinding. The
placebos are designed to be indistinguishable from the active drugs. Double-blinding is not
possible because subjects randomized to the riboflavin will have yellow urine (a harmless
outcome that will be explained to them).
Eligible participants will then be invited for a visit to the MRC Keneba field station. At
the initial visit, socio-demographic data and anthropometric measurements (height, weight,
waist and hip circumference and body composition by BIA) will be taken. Thereafter, BP will
be measured with an automated device in triplicate using a standard protocol by the same
investigator who will be blinded to genotype and treatment group. The investigators will also
collect 10ml sample of blood for laboratory assessment of vitamin B status. During the
intervention phase of the trial, the investigators will supplement participants with 5mg/day
of riboflavin or a matching placebo for 16 weeks. The pills will be supplied on a weekly
basis with instructions to return any unused pills. Another BP measurement following similar
protocol as before will be taken at 8 weeks as well as at 16 weeks after the start of the
intervention. Finally, a 10ml blood sample will be collected at 16 weeks. Blood samples will
be analysed for riboflavin, homocysteine, red cell folate, cobalamin and pyridoxine.
Participants who were randomized to receive placebo will be offered riboflavin
supplementation at the end of the study.
The investigators will use multilevel modeling test for a main effect of intervention on
delta BP from baseline to 16wk (and repeated at 8wk) adjusted for sex and age. Chi-squared
test will be used to test for changes in frequency of raised BP (>140/90). Then the
investigators will test for effect modification according to MTHFR variant.
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