Asthma Clinical Trial
Official title:
Management of Asthma in School-age Children on Therapy
Asthma affects 1 in 8 children in the UK. Up to half of these are treated with preventative
medicine in the form of low-dose steroids using an inhaler. The National Asthma Treatment
Guidelines recommend when this treatment is not working other treatments are started. Studies
to support this have taken place in adults but not with children. If patients are instructed
how to use inhalers and are given information about asthma, they can control their disease
much better. The first part of this study, lasting 4 weeks, will make sure the children and
their families understand how to use their inhaler. All children will be given the same
steroid inhaler to use and after 4 weeks those still with symptoms will enter the study
proper which lasts for 48 weeks. During this part of the study the children will be given one
of three treatments. These are:- a steroid inhaler + a dummy tablet, an inhaler containing a
steroid and a long-acting reliever + a dummy tablet or a steroid inhaler + an active tablet.
In this way the patient, the family and the researchers will not know which of the three
treatments the child is taking until the code is broken at the end of the study.
What matters to children is how they feel, are they able to run around and play with friends
and are they well enough to go to school. The investigators will assess which of the above
treatments best allow these to happen by asking the parents and children to fill in
questionnaires on 4 occasions during the study. The investigators will also see which
treatment best prevents the need for short courses of steroids tablets during the study.
These are commonly given when asthma symptoms worsen.
Most children will be started in the study through their general practitioner clinic. It will
take one year to enroll all 900 children. Once enrolled the children will be followed-up in
hospital centres. Much of the funding will be required to recruit and follow-up the children,
train everyone to the same standard and develop and administer the questionnaires and health
economic assessments. Asthma care is an expensive. The investigators will look at the costs
and assess which treatment offers most benefit. The team has experience and ability in this
field and will ensure the results are well publicised. Any child can withdraw from the study
at any time.
Asthma remains the most common medical condition seen in children in primary care and the
most frequent cause for medical paediatric hospital admission. It affects 1 in 8 children
nationwide, approximately 50% of whom are prescribed low-dose inhaled corticosteroids (ICS).
When treatment with low-dose ICS fails to control asthma symptoms, the National Guidelines
suggest ensuring compliance, maximising inhaler technique and giving appropriate information
about the disease to children and their families. Once these measures have been established
and if asthma symptoms persist, the Guidelines recommend changing the treatment (Step 3 of
the National Guidelines). The evidence at this step of the Guidelines is much weaker in
children than it is in adults. The reasons for this are that few studies have been undertaken
in children and most that have taken place have used adult-based outcomes such as lung
function measurements. This is unsatisfactory because we know that as a chronic disease
entity asthma in children is much more variable than in adults and between periods of
symptoms, lung function is often normal. Pharmaceutical company studies have really only been
conducted as part of their requirements to obtain a license to market their product. These
studies have generally been of short-term duration. They have not added to clinicians'
understanding of how and where to use the medications. They have not necessarily selected a
representative population due to their entry criteria and their intensive study requirements.
Such requirements mean that "real-life‟ compliance does not occur. In the independent
National Dutch Study which attempted to enter patients uncontrolled on low-dose ICS, three
treatment groups were employed: inhaled corticosteroids alone, inhaled corticosteroids in
double the dose and inhaled corticosteroids + a long-acting beta2 agonist. There was
essentially no difference in outcome measures between the three treatment groups as once
again the primary outcome measure was that of lung function (FEV1). Comparing this study with
a similar adult study6 both of which used lung function as the primary outcome measure, the
mean FEV1 on entry into the paediatric study was approximately 89% expected for the
children‟s heights. In the adult study the mean FEV1 on entry into the study was 74%
expected. It is therefore not surprising that the paediatric study was unable to show any
differences between the treatment groups.
We do not have the scientific information about how to treat children with asthma who are not
well controlled on low-dose ICS therapy. It used to be recommended that when low-dose ICS
were not effective their dose should be doubled. Studies in children, however, have
investigated this statement and the results are not impressive7 . There is no scientific
evidence that when control is poor in children with asthma, the dose of the inhaled steroid
should be increased. We have therefore decided not to introduce into this study a treatment
limb with a higher ICS dosage. There is anecdotal information, however, from many studies
undertaken within the pharmaceutical industry that when children enter a study which is
controlled and double-blind in nature, up to 30% of them improve, their symptoms reduce and
their lung function increases8. It is therefore surprising that approximately one third of
children receiving ICS are prescribed high-dose inhaled steroid therapy (≥ 800micrograms and
unlicensed beclometasone dipropionate or equivalent) or they are commenced on "add-on‟
therapies such as long-acting beta2 agonists (LABA) or leukotriene receptor antagonists
(LTRA) in addition to low-dose ICS. Concerns about the safety of high-dose ICS have been
raised in relation to growth impairment9, hypoglycaemia10 and suppression of the adrenal
cortex11 resulting in warnings on prescribing from the Medicines & Healthcare Products
Regulatory Agency (MHRA) in the UK12 and from the Food and Drug Administration (FDA) in the
USA. It is therefore unacceptable that approximately one third of children with asthma are
being treated with the above regimes. Asthma is a very common condition and the worth of
these regimes has not been proven by appropriately devised paediatric studies. The National
Guidelines have been developed in a "stepwise‟ manner, the amount of medication increasing at
each step if symptoms are not controlled.
However, as stated above, it may be that childhood asthma differs from that in adults. It
seems that relatively poorly controlled asthma in children who exhibit frequent symptoms do
not necessarily show abnormal lung function between their periods of symptoms. It is for this
reason that in our study we will be concentrating on outcome measures such as exacerbations
and quality of life although we will have the opportunity to measure spirometric values at
the first (T0) and last (T48) visits in the randomised part of the study. It could be that an
increase in medication may only be needed for a short time in children with asthma and there
have been suggestions that once control is achieved children should have their add-on therapy
reviewed. To incorporate such a step within the present study would make it excessively
complicated and would have major implications on the number of patients included. The
inclusion of such a step would make the study impractical within the UK. A study is needed
which is simple, pragmatic (but placebo-controlled and double-blinded), has outcomes which
will be of practical benefit to children and will provide evidence for the use of add-on
medications in the most cost effective and efficient way. Children dislike exacerbations.
School attendance, daily activity and general well-being increase when asthma is well
controlled. Once families understand sufficiently about asthma, inhaler technique has been
evaluated and optimised, and compliance issues addressed, one of the reasons why a specific
medication may be less effective could be related to the genetic make-up of the patient. In
this study we will have the opportunity, through a separate consent process, to collect and
store DNA specimens from saliva for later analysis of specific genetic polymorphisms in
relation to asthma severity and outcome. This aspect will bring added value to the study.
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