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[Back to edition-5] Introduction by Professor Bob Williamson, FRS, University of Melbourne
I hope that all of those affected by cystic fibrosis will take the opportunity to read the following summary of the article by Chris Boyd, (and the full article on line) even if it may be a bit complex for non-scientists, because it discusses all of the new approaches being studied worldwide. Published in this issue is a summary of these approaches and CFW will be publishing updates on developments as they become available.
We, like you, live in the "world of cystic fibrosis"
all the time, and are totally involved in trying to make things
better for those with CF. I am sure that every adult living with
CF knows that each group of doctors and scientists is committed
to its own favourite approach. The article by Boyd reminds us that
there are lots of approaches, not just "gene therapy"
or "ion transport modifiers" or "better antibiotics".
Indeed, in the 25 years that I have worked on CF, the improvements
have come from small advances in many different areas, each of which
can be more or less important for any individual living with CF.
Many of the children I knew with CF are now adults, working productively,
and while no one would pretend that life with CF is a bed of roses
(even 65 Roses), it is much improved on what it was, both in quality
and in time.
As the initiator of the first liposome CF gene therapy trial, carried out in London in the early 1990s, I am (of course) disappointed that all of us underestimated the problems that we would encounter introducing a healthy gene into the lungs of a patient with CF. This "gene therapy" approach is only just beginning to yield positive results, and probably will have to be combined with new stem cell and genomic approaches, perhaps in infancy or even in the womb. However, we all can be pleased at the fact that better mucolytics, better antibiotics, better treatment for immuno-rejection and better anti-inflammatory drugs all help with therapy in the here and now. The CF charities and research groups should be complimented and supported for trying such a wide range of approaches, because this ensures that things will continue to improve for everyone living with CF, perhaps not dramatically, but steadily over the years to come.
This article is dedicated to the memory of Sam Hillyard, who originally commissioned it.
A Christopher Boyd PhD
UK CF Gene Therapy Consortium
Medical Sciences (Medical Genetics)
University of Edinburgh
Molecular Medicine Centre
Western General Hospital
Crewe Rd
Edinburgh
EH4 2XU UK
Updated January 2005
Summary
Great strides have been made in our understanding of the underlying
basis of CF at the cellular and molecular level. This article examines,
from the point of view of a scientist, how these advances are being
translated into the clinic to treat CF lung disease, both through
conventional drugs and gene therapy.
Introduction
“Our knowledge is by
no means complete, and many more details need to be worked
out.” |
Although the life expectancy for patients has increased over thirty-fold
since 1940, we still lack a truly effective treatment for CF in
the airways. Why is this? One reason is that the root cause of the
disease was unknown until the discovery of the cystic fibrosis trans-membrane
conductance regulator (CFTR) gene by Lap Chee Tsui and colleagues
in Toronto in 1989. It then became apparent that the primary molecular
defect in CF was a faulty protein which normally acts as a chloride
channel. But that was only the beginning: it has taken all the intervening
years to build our present understanding of how this microscopic
fault leads to the infected and damaged CF lung over time. Our knowledge
is by no means complete, and many more details need to be worked
out. The prevailing idea is that defective CFTR leads to absorption
of water from the liquid covering the airways: this thin but sticky
layer stops the cilia (tiny hairs that cover the inner lining of
the air sacs) from beating and thus prevents mucus clearance mechanisms
from operating effectively. As a result, inhaled particles become
trapped on the airway surface for a long time, and bacteria are
able to colonise and initiate lung disease.
There are two basic therapeutic approaches. We can either target
the lung problems (eg. attack microbial infection or attempt to
modify the mucus layer); or we can target the basic causes (eg.
either coax the faulty CFTR protein into working or bypass it by
gene therapy or other means). Therapies targeting the basic causes
are more desirable for the treatment of CF, but it is undeniable
that such treatments are difficult to develop.
Concept to clinic: a long haul
“…better coordination
of clinical trials internationally, may soon reduce the time
span of the process to 7-10 years” |
The greatest obstacle to the emergence of new drugs for any disease
is time. The template for pharmaceutical research has evolved over
many decades and falls into three stages: (i) drug development and
testing, (ii) clinical trials (Phases I, II, III and IV), and (iii)
approval by regulatory bodies. To translate a single drug from concept
to clinic has traditionally taken fifteen years and cost around
US$500 M. In addition, it must always be borne in mind that only
a tiny proportion of drugs that enter development and testing pass
muster and enter clinical practice. The good news is that modern
techniques such as high throughput screening (HTS), and better coordination
of clinical trials internationally may soon reduce the time span
of the process to 7-10 years and reduce the cost several fold. Indeed,
the US Cystic Fibrosis Foundation (CFF) is pioneering this approach
in its Therapeutics Development Program started in 19981. Technological
advances enabled the rapid testing of thousands of compounds per
day. The CFF began to foster this technology in 2000 with grants
direct to pharmaceutical companies (eg. Aurora Biosciences) and
also direct grants to academic sites Alan Verkman's group, supporting
major drug discovery and development programs. At the beginning
of 2004, the CFF had an interest in 9 pre-clinical studies using
animal models and 14 clinical trials with human subjects.
Treating the effects of CF
Symptomatic therapy in the lung can either be direct, targeting the bacteria themselves with antibiotics or vaccines, or indirect, limiting the effects of damage caused by bacteria or the inflammatory process. Here we consider both lines of attack.
Anti-bacterials
| “…we
need to prescribe antibiotics more prudently and monitor resistance
patterns routinely” |
The bacterium Pseudomonas aeruginosa is a major pathogen in the
CF lung. Pseudomonas management is crucial in CF care, and many
antibiotic-based approaches have been used to treat it. One of the
problems of delivering antibiotics by normal routes is that undesirably
high doses are required. In recent years, TOBI (Chiron Corporation),
a nebulised form of tobramycin, has entered clinical practice and
provides more effective Pseudomonas control by targeting the drug
directly to the lung. Another antibiotic product, Colomycin (Pharmax),
has also been used successfully in this way. The concern with all
antibiotics is the emergence of bacterial resistance. Recent UK
data suggest that resistance to the commonly used antibiotics in
Pseudomonas from CF lungs is worryingly high: we need to prescribe
antibiotics more prudently and monitor resistance patterns routinely
in order to conserve the benefits of antibiotics in the long term.
Another interesting new approach to tackling Pseudomonas in CF --
still in its preclinical phase -- is DNA-based vaccination. If proven,
infants could be injected with a DNA vaccine and gain long-lasting
immunity to the capacity of Pseudomonas to infect the lungs.
Dealing with CF mucus
Viscosity or stickiness of the airway liquid layer is a key feature
of CF, favouring the colonisation of bacteria and other pathogens.
Ironically, the presence of large amounts of DNA released by damaged
neutrophils (cells involved in lung defence that are present in
large numbers in CF) worsens viscosity in the CF airways. The belief
that therapies aimed at destroying DNA from damaged cells would
reduce this viscosity and hence improve mucus clearance has led
to the development and widespread clinical use of Pulmozyme (Genentech
Corporation). Pulmozyme is a recombinant (DNA that has been created
artificially.from two or more sources and incorporated into a single
recombinant molecule) form of human DNAse delivered by aerosol inhalation.
| “..making
slight modifications to existing drugs to improve their effectiveness,
is an important strategy” |
A more recent contender for this type of treatment is Nacystelyn (NAL), a derivative of the food supplement N-acetyl cysteine which has had a history of therapeutic use in the CF lung. In 2002, an international group led by Dr App reported on a trial of the effectiveness of NAL (inhaled as a dry powder) for treating impaired mucus clearance. NAL was seen to increase the water content of mucus -- a desirable property -- as well as making it less sticky. There were no serious side effects but it remains to be seen how well NAL performs in more extensive trials. This approach, of making slight modifications to existing drugs to improve their effectiveness, is an important strategy in pharmaceutical research that can short-circuit some of the lengthy development times.
Stimulating alternative ion channels
Dr Richard Boucher's group in North Carolina is researching drugs
that are able to stimulate chloride channels other than CFTR and
hence substitute for its defective function. Results of a study
of one candidate drug, INS37217, were reported in 2002. This drug
is the latest of a series of so-called P2Y receptor activators which
have the desired effect. What is new about INS37217 is that it appears
to be more stable (and hence can maintain its activity for longer)
in CF sputum than previous drugs of this kind. Intriguingly, it
increases both mucus production and ciliary motion. Clinical evaluation
of INS37217 is under way.
Anti-inflammation
| “…So
far AAT has been tested successfully in laboratory culture
of human tracheal sections” |
Inflammation is a key manifestation of CF, though its root causes
remain unclear. Neutrophils (white blood cells and a primary defence
against bacterial infection) are involved in the inflammatory response
that produces enzymes called proteases whose main function is to
damage bacteria. The airway epithelium (membranes lining the airways)
produces anti-proteases to prevent proteases from biting back and
damaging the lung itself. The huge excess of neutrophils in CF generates
too much protease for the lung's anti-proteases to deal with, and
lung damage unfortunately results. A therapy based on adding more
of a natural anti-protease called alpha-1-antitrypsin (AAT) has
been mooted as a way of restoring the balance. Recombinant AAT has
been shown to work when delivered as an aerosol but this approach
has many drawbacks. A more refined approach is being developed by
Dr Pam Davis and colleagues, in which AAT is attached to a targeting
protein such that (when delivered either as an aerosol or intravenously)
the AAT is ferried to the surface of epithelial cells and secreted
at the site of desired action. So far this has been tested successfully
in laboratory culture of human tracheal sections. Other groups are
working on alternative anti-protease strategies attacking the same
inflammatory defect. This mode of therapy has considerable promise,
but, should it reach the clinic, it is likely to be beneficial only
in individuals with early-stage disease.
| “…
The prominent non-steroidal anti-inflammatory drug ibuprofen
has undergone a trial in CF patients with encouraging results” |
Recently there has been much interest in non-steroidal treatments
of CF lung inflammation that avoid the side effects associated with
corticosteroid treatment. The prominent non-steroidal anti-inflammatory
drug ibuprofen has undergone a trial in CF patients with encouraging
results: the rate of decline in lung function was reduced. However,
there has been a report of undesirable toxicity when ibuprofen was
used for CF in conjunction with an antibiotic of the aminoglycoside
class. Clinicians will remain wary of using ibuprofen for CF until
a means of avoiding such toxic interactions is thoroughly understood.
Finally, the anti-inflammatory properties of antibiotics called
macrolides have been increasingly evaluated in CF. These drugs may
work at several different levels. For example, the macrolide clarithromycin
has been shown to disrupt the biofilm environment proposed to favour
Pseudomonas growth in the infected lung. There has been a surge
of interest in azithromycin in particular, whose use in CF was inspired
by its success in treating diffuse panbronchiolitis. Several trials
showing promising results on CF lung function have taken place.
However, the mode of action of macrolides in CF is still not clear,
though their anti-inflammatory properties are thought to dominate.
The results with azithromycin have been encouraging enough that
we are beginning to see its use recommended under certain conditions
in CF patients as an adjunct to more established therapies. We are
still some way from a consensus on its efficacy and long term randomised
controlled trials with large numbers of patients are required to
determine its efficacy and optimal dosage with precision.
Treating the basic causes of CF
The attraction of therapies that target CFTR is that
they have the potential to compensate for all the symptoms associated
with the defective protein. Almost all therapies of this kind are
still in their early developmental stages. It is important to remember
that many compounds that work well in laboratory experiments and
simple model systems in many cases do not translate to useful drugs
in living animals, due to toxicity and other undesirable effects.
CFTR as a drug target
Our detailed knowledge of CFTR is being applied in the search for
therapeutic drugs that improve the function of defective CFTR or
(as we have seen) stimulate the activity of other proteins that
may substitute for it. Some drugs emerged early on in the CFTR story
and are still invaluable for laboratory research, but have not progressed
to clinical use. Genistein, an activator of CFTR, is a well-known
example. Genistein could yet play a clinical role: a proposed trial
of a combination therapy comprising phenylbutyrate and genistein
at the Children's Hospital of Philadelphia is recruiting patients
(NLM identifier NCT00016744).
In the last few years, Dr Freedman and others in the US raised the
possibility that docosahexaenoate (DHA) which is a polyunsaturated
fatty acid, given as a dietary additive, could be used to treat
CF. This followed published evidence that the DHA/arachidonic fatty
acid imbalance in CF cells could be corrected by this means. However,
the work remains in the pre-clinical phase and initial excitement
about this approach has declined significantly.
The F508del mutation
| “There
are several experimental drugs that appear to mobilise F508del-CFTR” |
Most CF patients have the F508del variant of CFTR, so it is not
surprising that a great deal of attention has been focused on the
properties of this protein. So-called protein-mobilising drugs that
mimic the beneficial effects of growth in the cold are being actively
sought. Such a drug may not be sufficient, however, because when
F508del protein does reach the cell surface in patients it is less
functional than normal CFTR. We may need to find F508del activity-enhancing
drugs as well.
There are several experimental drugs that appear to mobilise F508del-CFTR.
These include MPB members of the benzo(c)quinolizinium family. Dr
Bob Dormer and colleagues in Cardiff in collaboration with Dr Fred
Becq's group in Poitiers have shown that treatment of F508del nasal
cells with MPB compounds results in better delivery of CFTR to the
cells' upper surfaces. Under certain conditions the same compounds
were also able to stimulate chloride channel function.
Another drug with reputedly similar beneficial effects on F508del
cells is thapsigargin, a calcium pump inhibitor, as reported in
2002 by Dr Marie Egan and colleagues at Yale. This work is somewhat
at odds with other published data that suggest thapsigargin acts
to inhibit proper processing of proteins. Dr Egan argues that some
proteins, including F508del-CFTR, are exceptions to this rule. We
await clarification of the effects of thapsigargin on F508del-CFTR
with interest. A related compound, curcumin, which is a component
of the natural food additive turmeric, was reported by Dr Egan and
colleagues in 2004 to correct F508del-CFTR defects in mice. Unfortunately,
in a Phase 1 study in patients, no effect on F508-del CFTR was seen.
Furthermore, scientists in other laboratories have been unable to
replicate the effects of curcumin in mice.
High throughput screening methodologies (see below) offer the possibility
of vastly increasing our repertoire of protein mobilizing drugs.
Other mutant forms of CFTR
Not all attention is focused on F508del-CFTR: much research
is devoted to discovering and analysing drugs that activate whole
classes of mutant forms of CFTR. For example, Dr David Sheppard
and colleagues in Bristol are studying phloxine B and similar compounds
that belong to a family of commercially-used food dyes. In early
studies, these compounds have been shown to activate and inhibit
CFTR in cell culture systems. This class of drugs is particularly
attractive because it is already in use in food, its lack of toxicity
is already known which therefore offers the prospect that future
trials may be less protracted.
High Throughput Screening (HTS)
| “Dr Verkman's
group and others are scaling up HTS efforts by screening over
100,000 compounds, to search for drugs that can activate or
mobilise defective CFTR.” |
As an example of HTS, Dr Alan Verkman and colleagues in San Francisco
are undertaking a CFF-funded drug discovery program. In their first
study, hundreds of flavone and benzoquinolizinium derivatives were
screened in a special cell system designed to detect drugs that
affect CFTR activity. Certain 7,8-benzoflavones were shown to be
most active; one in particular was found to be a potent inhibitor
of CFTR activity. While this drug is not applicable to CF patients,
it will be a useful addition to the armory of drugs available for
laboratory research. There is also a possibility that it could be
used in the clinic to treat conditions such as cholera. After this
promising start, Dr Verkman's group and others are scaling up HTS
efforts by screening over 100,000 compounds, to search for drugs
that can activate or mobilise defective CFTR. Much progress has
been made, and an inhibitor of CFTR has been identified that may
have a role in the treatment of cholera. Lead compounds that activate
or mobilize CFTR in vitro are currently being evaluated in vivo.
It is too early to say whether any of them will find clinical application.
Modifier genes
| Identifying which
genes might be able to modify the CF defect is another major
area of research, one that has benefited tremendously from
the genome mapping projects undertaken in the last decade. |
As with many other genetic diseases, CF progression varies between
individuals. The environment has a major effect on variability,
but the genetic make-up of the patient is also important. Why, for
example, do some F508del patients become severely ill early in life
and others remain healthy into middle age and beyond? We know that
there are genes for proteins that :
(i) interact directly with CFTR,
(ii) act as ion channels,
(iii) take part in the inflammatory response and
(iv) have direct anti-bacterial activity.
Such genes and others are potential modifier genes, affecting the
severity of disease progression. As a hypothetical example, suppose
there is a gene X responsible for an ion channel P. X might exist
in two forms, one producing a more a more beneficial version of
P than the other. Patients who happen to have inherited the more
beneficial version of X might then experience less severe symptoms
because the more active P is able to compensate in part, for the
CFTR defect.
| “ Any CF
modifier genes and proteins confirmed as human-relevant will
provide new drug targets, and thus significantly widen the
scope of CF drug development” |
The mouse has proved to be an invaluable tool by use of which modifier genes can be rapidly identified using carefully-designed breeding programs. In addition, genomics and proteomics -- whole disciplines devoted to new ways of looking at the expression patterns of large numbers of genes and proteins simultaneously, facilitate the identification of such genes. Once a modifier gene has been identified in the mouse, its relevance to the disease in humans can be tested by analysing the equivalent human gene in families and especially in twins with CF. Any CF modifier genes and proteins confirmed as human-relevant will provide new drug targets and thus significantly widen the scope of CF drug development.
Gene therapy
| “…early
attempts to transfer the normal gene into patients (delivered
either by a modified virus or by a synthetic carrier) proved
disappointing” |
CF gene therapy consists of delivering normal CFTR genes (usually
in the form of DNA) into the affected airway cells of patients where
they can produce undamaged CFTR protein and hence restore cells
to normal working. As soon as the CFTR gene was discovered, the
concept of gene therapy for CF was enthusiastically promoted and
many groups worldwide took up the challenge of developing it. It
was thought that CF was an ideal disease to treat by gene therapy
for two main reasons. Firstly, the affected tissue, the lining or
epithelium of the lung airways, was readily accessible, and secondly,
it was believed that replacement of only about 5% of normal CFTR
function would be sufficient to correct the defect. Both these reasons
remain valid, but early attempts to transfer the normal gene into
patients (delivered either by a modified virus or by a synthetic
carrier) proved disappointing. Trials provided evidence that the
process was safe, that the gene was getting into lung cells, and
that functional CFTR was being made: but production levels were
low and the normal gene stopped working after a few days.
It is now clear that the lung epithelium presents a series of impressive
barriers to gene therapy, barriers that have evolved over millions
of years as defense systems to ward off invading pathogens and keep
the lungs clear and healthy for gas conductance and exchange. As
far as the epithelium is concerned, gene therapy complexes represent
just another class of invaders that need to be repelled. The short-lived
gene expression seen in early trials revealed one aspect of lung
defense that has evolved to switch off the genes of malevolent intruders
such as viruses. The CF lung is an even more formidable target,
because the sticky mucus layer physically traps many kinds of gene
therapy complex and prevents their efficient entry into cells.
| “…modified
viruses have been the most used carriers or vectors for delivering
normal CFTR in gene therapy” |
The greatest challenge for CF gene therapy research therefore involves
efficiently breaching these barriers. We have learnt much from viruses
such as adenovirus, which have evolved efficient means of entering
cells. Indeed, modified viruses have been the most used carriers
(or vectors) for delivering normal CFTR in gene therapy. However,
until we solve the problem of keeping the introduced gene working
for a long time, we are going to need to deliver gene therapy complexes
at regular intervals. The efficiency of the immune system (even
in CF patients) at building up immunity over time means that viruses
cannot currently be used as carriers for this purpose. Also, serious
adverse effects have been reported recently in (non-CF) gene therapy
trials involving viruses. Because of these and other perceived drawbacks
of viruses, more effort is currently being expended towards developing
non-viral or synthetic means of delivering the CFTR gene. The main
drawback of non-viral delivery methods is their relative inefficiency,
but new methods, including the addition of small pieces of protein
that allow the complex to home in on epithelial cells, are being
developed. By such means and others, we are beginning to increase
delivery efficiency and expect to devise effective formulations
in the foreseeable future.
Recent developments
| “ results
have just been published in full, confirming partial reconstitution
of CFTR function” |
Two gene therapy trials in the US have reported recently. In one,
a Phase II trial, a recombinant adeno-associated virus carrying
CFTR was administered to the maxillary sinuses of 23 patients with
antrostomies (an opening in the sinus for the purpose of drainage).
While the treatment was safe and well tolerated, most of the endpoint
measurements showed no statistically significant changes, and it
is difficult to conclude that the intervention had a positive effect.
In the other trial (Phase I), a proprietary non-viral formulation
containing compacted DNA nanoparticles, was used to deliver CFTR
to the noses of 12 patients. There were no significant side effects
and interestingly, as in some earlier nasal trials, there was a
trend towards correction of the potential difference defect in a
proportion of treated patients. The results have just been published
in full, confirming partial reconstitution of CFTR function. Further
studies of this interesting formulation are being carried out.
New approaches to CF gene therapy
| “This ambitious
initiative has allowed us to combine forces to evaluate and
devise new approaches to CF gene therapy” |
The CF Trust has set up the UK CF Gene Therapy Consortium (UKCFGTC)
which combines the research efforts of three leading CF gene therapy
centres in Oxford University, London (Imperial College) and Edinburgh
University with the express aim of developing effective formulations
for clinical use. This ambitious initiative has allowed us to combine
forces to evaluate and devise new approaches to CF gene therapy.
We are focused on initiating a clinical trial in 2006, and pre-clinical
testing of a range of gene transfer agents is under way. Other approaches
being studied by the UKCFGTC, some more futuristic, are described
below.
How can long term CFTR production be achieved?
As mentioned above, the first generation of gene therapy vectors
functioned for only a short time. Consequently, improvement in vector
design is necessary in order to establish long-term clinical benefit.
My group in Edinburgh is constructing and testing large vectors
with much more of the natural CFTR gene than is present in conventional
vectors, in the expectation that more sustained expression (with
a higher degree of cell and tissue specificity) will result. Currently
we are beginning to improve delivery efficiency, and plan to test
these vectors in vivo.
An important finding from early non-viral gene therapy trials was
that the DNA used, being of bacterial origin, was recognised as
alien by lung cells and triggered a specialised defence mechanism
resulting in inflammation. We now understand what features of the
DNA induce this mechanism. For immediate application, UKCFGTC scientists
in Oxford are therefore developing small vectors with improved CFTR
gene sequences that are designed to produce CFTR in a sustained
and non-inflammatory fashion.
Stem cells
| “…spectacular
recent advances in stem cell research lead us to believe that
the approach is worth pursuing, although it is likely to be
a longer term goal” |
One idea being investigated is stem cell based therapy. Stem cells
are progenitor (ancestor) cells that are believed to exist in most
organs, including the lung, and divide when called upon to replace
dead or dying cells. The aim is to isolate and grow stem cells from
patients' lungs in the laboratory, during which time the normal
CF gene can be inserted. Corrected cells could then be put back
into the patient where they would establish themselves in the appropriate
airway region. If sufficient numbers of corrected stem cells could
be induced to bed down in this way, they could provide a permanent
supply of epithelial cells producing normal CFTR, and hence alleviate
the disease. We do not presently know how we might achieve this
in practice, but spectacular recent advances in stem cell research
lead us to believe that the approach is worth pursuing, although
it is likely to be a longer term goal. We are encouraged by the
success of bone marrow based gene therapy, which has proved efficacious
in the treatment of babies suffering from a fatal condition known
as X-linked SCID.
Electroporation
As we have seen, delivering DNA to lung cells is difficult. One
way of providing the energy to force DNA into cells is a method
called electroporation, in which short pulses of electric current
are used to punch tiny holes in cells allowing DNA to enter. This
has been used in the laboratory setting for years, but now researchers
have shown that this method can work in vivo. The challenge is to
develop suitably safe and effective means of carrying out procedures
such as electroporation in the lungs of patients. The UKCFGTC is
investigating whether electroporation is a feasible way of enhancing
gene therapy delivery to the lung. This is just one of a variety
of physical methods to aid in gene delivery being assessed by the
UKCFGTC.
Repairing the defective gene
| “…proof
that the technology works is a necessary first step towards
improving its efficiency” |
Rather than supplying an entire working copy of the CFTR gene,
there has been much effort recently towards repairing the mutant
gene itself. In brief, the concept is to deliver a small "patch"
of normal CFTR DNA which could provide the template for the cell
machinery to repair the mutated part of a resident CFTR gene. This
method works to varying extents in the laboratory, but UKCFGTC and
other scientists have found its efficiency in epithelial cells to
be immeasurably low. While the method remains attractive in principle,
a clear demonstration that efficiency in the target cells can be
vastly improved must be found before we can revisit this approach
to CF gene therapy.
A parallel approach by Dr Engelhardt and colleagues in Iowa has
been to correct CFTR mRNA rather than DNA. (The cell makes a message
or mRNA copy of the DNA of each gene which it then processes to
make protein.) Using a highly complex procedure, they were able
to correct the F508del mutation both in cells and in mice. The efficiency
is currently too low for in vivo clinical application. However,
it may find clinical application as part of a stem-cell based therapy.
Conclusion
| Many believe
that a multi-pronged treatment, combining drug and gene therapy
elements, will succeed.” |
Persuading big pharmaceutical companies to invest large sums into
developing therapies for CF (which is, after all, a relatively rare
disease) is difficult. CF's orphan status means that charity-funded
and academic-based groups are bearing much of the burden of necessary
work. Nevertheless, all the high-tech paraphernalia of drug and
gene therapy development are being harnessed enthusiastically for
the treatment of CF. The US CFF is actively promoting intensive
research into new drug discovery. Candidate compounds with exciting
properties have already emerged and more are certain to be produced
in the near future. Drugs that mobilise F508del-CFTR in an active
form to the cell surface in vivo are most eagerly awaited.
For all the reasons discussed above, gene therapy has proved to
be more difficult to develop than initially hoped. In the last few
years, however, there have been notable gene therapy successes for
other diseases, and more focused research such as that being undertaken
by the UKCFGTC will accelerate progress. Achieving efficient delivery
to lung cells is the trickiest challenge, but one or more of the
new physical delivery methods being assessed may help us reach the
threshold of efficiency required to bring clinical benefit.
It is impossible to predict whether effective treatment of CF lung
disease will eventually be drug-based or gene-based: both approaches
have advantages and difficulties. Many believe that a multi-pronged
treatment, combining drug and gene therapy elements, will succeed.
Organisations such as Cystic Fibrosis Worldwide and national CF
societies have a major role to play in encouraging the multi-centre
coordination of clinical trials that will be necessary to speed
the assessment of all new therapies. They also provide valuable
forums in which clinicians, scientists and patients can meet and
exchange views on how to advance our treatment of CF.
Acknowledgements
Thanks are due to the UK CF Trust for supporting my research,
and to colleagues in the CF research community (especially those
in the UK CF Gene Therapy Consortium) for helpful discussions .
A Christopher Boyd PhD
UK CF Gene Therapy Consortium
Medical Sciences (Medical Genetics)
University of Edinburgh
Molecular Medicine Centre
Western General Hospital
Crewe Rd
Edinburgh
EH4 2XU UK
Updated January 2005
Editor’s notes:
For a list of references for this article please contact us
at
editor@cfww.org
The following web pages are supplied for readers interested in further information about specific drug trials:
http://www.cff.org/research/cystic_fibrosis_foundation_therapeutics/
therapeutics_devl_network/
http://www.clinicaltrials.gov/show/NCT00016744)
http://www.cff.org/news/press_releases.cfm?ID=85