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Radical
Prostatectomy
- Keyhole
Surgery
Radical Radio Therapy
- Brachytherapy
Active Surveillance
Watchful Waiting
Hormone Manipulation
Orchidectomy
Cryo-ablation Therapy
Vaccine
Bone Integrity
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Treatments
Please note. We do not endorse
any of the treatments listed and
cannot make any medical
recommendations, or give medical
advice.
Radical
Prostatectomy
This
is one of the two main radical
treatments for Prostate Cancer
offered in the UK at the present
time for patients mainly under 70
years old. In the USA it is the
main form of treatment. It is
regarded as too risky for most
patients over 70, and as prostate
cancer is usually slow growing,
other treatments are considered
more suitable.
To remove the whole prostate is a
major operation, you will expect
to be in hospital for about a week
and you will have a catheter in
place for 3 - 4 weeks.
Very occasionally at the start of
the operation the surgeon will
find the cancer has spread beyond
the prostate and in these cases he
may not remove it.
Most men will suffer some urinary
incontinence after the operation
but this will improve. A very few men
will have permanent incontinence
problems. Most men will suffer
some degree of impotence after the
operation, but this may be short
lived.
There is a risk of high blood
loss during the operation, and
like any major surgery there is a
one per cent chance that you may
not survive it.
However if all goes well you
probably have the best chance of a
cure with this treatment.
By courtesy of the Covent Garden
Cancer Research Trust
(illustrations by Diane
Mercer).
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Laparoscopic (Keyhole)
Surgery
There have been several
recent advances in the UK in
laparoscopic (keyhole)
surgery.
This technique requires 5
small ½ inch incisions in the
abdomen, Carbon dioxide is
pumped in and this lifts the
abdomen wall so that the
surgeon gets a better view of
what is happening, instruments
are then inserted through
narrow hollow tubes placed in
the incisions. The surgeon is
then guided by the laparoscope
(camera) which is inserted
through the remaining
tube.
The advantages of laparoscopy
are fairly well known,
· It can shorten your stay in
hospital, 50% of men are
discharged after one day.
· There is significantly less
bleeding.
· You are less likely to need
pain killers when you leave
hospital.
· Usually the catheter is
removed one week after the
operation.
· Approx. 90% of men can
return to work two to three
weeks after the operation.
The main disadvantage is that
the laparoscpic operation may
well take twice as long on the
operating table as the
traditional open surgery
method.
Studies from Europe and the
US suggest that the rates of
prostate cancer recurrence are
the same for both techniques
as is the incidence of
impotence and
incontinence.
One interesting index which
is used to assess the
effectiveness of a Radical
Prostetectomy, either
traditional open surgery or
laparoscopic is the 'positive
surgical margin.' This
measures the presence of
cancer cells at the cut margin
of the removed prostate. The
best result worldwide is
around 20%. The reason one
cannot get much lower than
this is because 2/3rds of
cancers occur in the periphery
of the prostate. In the UK
both traditional open and
laparoscopic surgery averages
out at about 30%, the reason
for the higher figure is that
in the UK prostate cancer is
operated on at a later stage
than in the US and Europe,
presumably due to a lack
awareness and screening.
There are two variations of
the Keyhole technique the
first is where the surgeon
operates by hand using the
laparoscope. This is conducted
at the North Hampshire
Hospital Basingstoke (over 100
operations) and also at Kings
College Hospital and Southmead
Hospital Bristol (smaller
numbers). The second variation
is where the surgeon uses a
robot to carry out the
operation which he can operate
from another room or in theory
even another town. This is
conducted at St Mary's
Hospital Paddington.
For further information see
the websites available in the
links
section.
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Radical
Radiotherapy
This
is an alternative to a Radical
Prostatectomy and is the other
main form of treatment for
prostate cancer in the UK at the
present time. The treatment is
administered daily over a 4 - 6
week period as an outpatient at a
hospital. Each session lasts only
minutes but on each occasion you
will need to be positioned on the
equipment very carefully. The
effect of the treatment is
cumulative and some patients will
have difficulty lasting the full
course.
By courtesy of the Covent Garden
Cancer Research Trust
(illustrations by Diane
Mercer).
Side Effects
The main side effect is
irritation or pain to the
bladder and/or rectum. This
will usually subside within 4
- 6 weeks after the treatment
but in many cases it will need
medication.
Very occasionally there will
be long term damage to the
bladder or rectum resulting in
incontinence.
Some men will suffer from
impotence after the treatment
and lose their sex drive.
Associated Treatments
1. Hormone Treatment
It is fairly common to be
given Hormone treatment before
commencing radiotherapy as
this will shrink the prostate
and make it more easy for the
radiation to work.
In addition a course of
hormone injections is some
times given after the
treatment for 6 - 18 months.
This will help to starve any
remaining cancer cells and
keep the PSA count low.
2. Conformal Radiotherapy
This is an alternative to the
standard treatment mentioned
above it is only practised at
a few hospitals and requires
special equipment. The
equipment focuses the beams
more precisely so that they
can be aimed directly at the
cancer. This enables a higher
dose of radiation to be given
and provided it hits the spot
it can be more effective and
have fewer side effects.
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This
is another alternative to Radical
Radiotherapy now increasingly
available in the UK. The treatment
consists of inserting radio active
seeds into the prostate targeting
the cancer. These seeds do not
need to be removed because they
will loose their radioactivity
fairly quickly and become
harmless. This treatment avoids
the need to attend a Radiology
clinic on a regular basis but
suffers similar but milder side
effects as Radical
Radiotherapy.
Further
information on Brachytherapy is available on the Prostate
Brachytherapy Advisory Group website: www.prostatebrachytherapyinfo.net
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Active
Surveillance
Active surveillance of early
prostate cancer
Doctors from the Royal Marsden
Hospital are studying 'active
surveillance' in men with early
prostate cancer. They need to
recruit several hundred men.
If you are interested in the
research, see if you fulfill these
criteria, and then read a little
more about the study. If you want
more information, the contact
details of the Lead Researcher are
at the end. To join this study you
must be a man with prostate cancer
between the ages of 50 and 80 with
a Gleason Score of less than or
equal to 7 and a PSA of less than
15 who has not yet had treatment
and is within travelling distance
of The Royal Marsden in
Sutton.
Here is some information about
the background to the study.
Strange as it may seem, most men
with early prostate cancer do not
need to be treated. Usually, the
cancer grows so slowly that the
man will live out his natural
span, and die of something else,
before the cancer causes any
symptoms. Unfortunately, not all
early prostate cancers behave like
this. Over the years, some will
progress so the cancer causes
symptoms, or may even spread to
other parts of the body and become
life-threatening. Although we know
that most cases of early prostate
cancer will never need treatment,
at present we have no good way of
telling which will need treatment,
and which will not.
There have been two standard
approaches to this problem. The
first has been to recommend
aggressive treatment to all men
with early prostate cancer. This
means surgery to remove the
prostate, or a course of
radiotherapy. While this ensures
that all the significant cancers
are treated, it also means many
are treated when they don't need
to be. As the treatment can have
major side-effects, particularly
incontinence or impotence, this is
a big problem.
The second approach has been
described as 'watchful waiting'.
This means that men with early
prostate cancer are seen regularly
in clinic. If they develop
symptoms from progressive prostate
cancer, their doctors will start
them on hormone therapy. While
this approach avoids the
side-effects of surgery or
radiotherapy, it may be 'under-
treatment' for some men.
Active surveillance
We want to study 'active
surveillance' as an alternative
approach which aims to identify
the minority of men with early
prostate cancer who need to be
treated with surgery or
radiotherapy, so that the
remainder are spared the
side-effects of unnecessary
treatment. Men on active
surveillance are closely monitored
with a PSA blood test every few
months, and repeat sampling of the
tumour every 2 years. Those men
whose cancer shows signs of
progressing receive aggressive
treatment, either with surgery or
with radiotherapy. Those men whose
cancer remains stable continue to
be monitored. This means they
avoid the risk of treatment
side-effects. Whereas watchful
waiting is relatively lax
observation with late, gentle
treatment in reserve for symptoms
of cancer progression, active
surveillance involves close
monitoring with early, aggressive
treatment in those with subtle
signs (but no symptoms) of cancer
progression. Early results from
Canada, based on over 200 selected
men with early prostate cancer,
suggest that as many as 70% of men
on active surveillance will avoid
treatment for their prostate
cancer.
Here is some information on the
study itself
Men have a PSA blood test every 3
months for the first 2 years, and
every six months thereafter. If
willing, they also have a prostate
biopsy every 2 years. Men who are
on active surveillance may also
take part in one of several
related studies designed to
identify predictors of prostate
cancer behaviour (for example we
are studying the idea that the
tumour oxygen levels may be an
important determinant of prostate
cancer behaviour) or to test novel
therapies designed to slow the
rate of cancer progression.
The study is funded in part by
the National Cancer Research
Institute Prostate Cancer
Collaborative. If you think you
would like to find out exactly
what is involved please
contact:
Dr Chris Parker, Senior Lecturer
and Honorary Consultant in
Clinical Oncology,
Academic Urology Unit,
Royal Marsden Hospital,
Orchard House,
Downs Road,
Sutton, Surrey, SM2 5PT
tel. 0208 661 3425; e-mail:
cparker@icr.ac.uk.
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Watchful
Waiting
As the name implies this is a
holding position. It involves
regular check ups to monitor
the cancer. You will need to
see the specialist every 6 to
12 months for a PSA test and a
rectal examination. No
treatment is involved unless
the cancer develops. Watchful
waiting is usually appropriate
for older patients of 70 years
or more.
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Hormone
Treatment
It is
fairly common to be given Hormone
treatment before commencing
radiotherapy as this will shrink
the prostate and make it more easy
for the radiation to work.
In addition a course of hormone
injections is some times given
after the treatment for 6 - 18
months. This will help to starve
any remaining cancer cells and
keep the PSA count low.
In addition Hormone Treatment is
often given as the main treatment
when the two radical treatments
are not considered suitable as is
sometimes the case with older
patients. The effectiveness of
Hormone Treatment can wear off
after two or more years and it
will then need to be changed or
stopped for a
while.
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Orchidectomy
An
Orchidectomy is an operation for
the removal of the testes,
performed under local or general
anaesthetic. It can be done as a
day case, or maybe an overnight
stay. There will be some pain in
the week after the operation,
which is usually helped by
painkilling tablets. Take things
easy in the first week and avoid
heavy lifting.
Because Testosterone is made in
the testicles, an Orchidectomy, is
a way of stopping its production.
This will help to stop prostate
cancer from growing and may even
cause it to shrink. Some men
prefer this operation, to taking
medication over a long period. If
you have been suffering from
cancer related pain, it will
relieved by an Orchidectomy in
most men for a period of time.
What are the adverse side effects
of this operation? An Orchidectomy
cannot be reversed, so you must
consider the following permanent
adverse side effects.
You will be impotent, or unable
to have an erection
You will lose your sex drive
You will be infertile
You will experience hot flushes
(this is due to hormonal
changes)
You will be left with little
tissue in your scrotum (you can
have implants to overcome
this)
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Cryoablation
Targeted
cryoablation of the prostate
(TCAP) is an innovative new
therapy for primary prostatic
cancer, localised to the gland,
and also for those men who have
recieved radiotherapy treatment
and then relapsed.
It has been in use in the USA for
5 years and data indicates it can
be as succesful as other treatment
modalities. It may be more
advantageous in those men with a
more aggressive type cancer. In
those men who have recurrent
cancer post irradiation results
indicate that up to 66% will be
tunour free at 2 years post
TCAP.
The treatment is based on
established cryosurgery
principles. Fine cryoprobes are
inserted into the prostate under
ultrasound control. This can be
under either general anaesthetic
or local anaesthetic. Temperature
monitors are used to accurately
measure local temperatures to
protect surrounding structures ie
bladder and rectum. The prostate
is totally frozen to -140C. The
thaw process utilises helium. The
urethra is protected by a special
urethral warmer.
Men are discharged with a small
catheter in situ for 3 weeks to
allow healing and the n
removed.
Side effects include incontinence
(1-2%) and impotence (70%)
although this recovers in over
50%.
Not all men are suitable for
TCAP. Those who have had a
transurethral resection (TURP)
have a high rate of incontinence
and are therefore not advised to
have TCAP. Large glands may also
not be suitable.
TCAP is targeted cryoablation of
the prostate. It differentiates
old cryo type approaches with
liquid nitrogen from new
technology with ultrasound and
argon.
A web site is under development
www.cryosurgery.co.uk
Mr John H. Davies Consultant
Urological Surgeon,
Royal Surrey County Hospital,
Guildford,
GU25XX
Tel 01483 571122 ex 4878
fax 01483 454871
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Vaccine
What is vaccination and
immunity?
Since Jenner's first
successful vaccine against
smallpox many successful
vaccines have been produced. A
vaccine is usually made from a
"weakened" form of a known
germ (pathogen). The weakened
form of a germ does not cause
illness. but the vaccine
teaches the body what the germ
looks like and protects the
person from ever becoming
severely infected by the
contagious form of the germ in
the future.
Can we have vaccines for
cancer? Cancers are not
contagious like the diseases
which spread through proximity
to other infected people and
through contaminated water,
but vaccines represent
important new therapeutic
treatments for cancers.
Scientists have been trying to
find ways of triggering an
immune response to cancerous
cells for many years, but
since the cancer cells are
part of the patient's own
tissue and not "foreign", the
immune system may be
"tolerant" and ignore them.
This is explained in the
article: "Smallpox, polio and
now a cancer vaccine?" Donald
W. Kufe, Nature Medicine Vol.
6 No. 3 March 2000. He says
that - "Advances in our
understanding of anti-tumour
immunity and the genetic
alterations that accumulate in
the progression to malignancy
have recently provided
unforeseen opportunities for
the development of more
selective and safer
approaches." More information
can be found at the web site
provided by CancerHelp UK,
http://medweb.bham.ac.uk/cancerhelp/public/
How are cancer vaccines
developed? Although, in the
future, vaccines may be
produced to prevent cancer,
research studies are
concentrating on developing
vaccines as a therapeutic
treatment for those who
already have cancer. The
approach sometimes adopted is
to use the patient's own
cancer cells to make the
vaccine. This is called an
"autologous" vaccine, and the
process requires laboratory
cultivation of the cells. This
painstaking laboratory work
can be conducted for a few
patients only. For this
reason, it is necessary to
develop "allogeneic" vaccines.
These are not made using the
patient's own cells, but from
related cancer cells, and
would allow a larger number of
patients to be treated.
Trials for prostate cancer.
The development of vaccines
for prostate cancer is
possible because of our
improved theoretical
understanding and laboratory
techniques. Treatment with
vaccines is usually a course
of several injections is given
under the skin, which may have
to be repeated to reactivate
the immune response.
Clinical trials are in
progress at many hospitals.
For example, those conducted
at Johns Hopkins University
School of Medicine on prostate
cancer patients showed
encouraging results, and
further trials are planned. Dr
Jonathan Simons has published
a report of this work in
Cancer Research 59, 5160-5168,
October 15 1999, and refers to
the web site:
http://www.cellgenesys.com
In addition trials have
recently started at St
George's Hospital Medical
School in south London with
Onyvax TMP. This is a
therapeutic vaccine designed
to provoke the immune system
to attack prostate cancer
cells. At this stage the trial
will enrol patients who are in
the early stages of the
disease, those who have tried
Hormone therapy but where the
PSA has again started to rise.
For further information phone
020 8682 9131 or use website
www.onyvax.com
How could genetic engineering
enhance the immune response?
Many techniques are being
developed, using genetic
technology. A piece of DNA may
be added to a cancer vaccine
to help make a marker visible
to the immune system, or
dendritic cells may be used,
taken from a patient, grown in
an incubator and treated with
some patient tumour cells to
teach an immune response
before returning these to the
patient. Another technique is
to inject cancer cells
combined with either foreign
bacteria cells such as BCG, or
a protein, to trigger an
immune response. Refer to the
Cancer Research Campaign and
Everyman at:
http://www.crc.org.uk/science/therapy3.html
and
http://www.icr.ac.uk/everyman/
What are the side effects of
vaccine treatment? Established
treatments for cancers, such
as chemotherapy, radiotherapy
and hormone therapy may have
serious side effects, and in
many instances are only
palliative. In contrast cancer
vaccines have so far caused
only mild side effects, like a
mild influenza. Vaccines
represent a more hopeful
methodology for producing
effective treatments, and are
less physically taxing for the
patient than the multiplicity
of drug therapies applied
using a pragmatic
approach.
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Bone
Integrity
Bone Integrity and Prostate
Cancer - Beginning The
Debate.
A review by Roy Nixon
Unfortunately for men with
prostate cancer, cancer cells
are often attracted to bone.
As if this was not bad enough,
androgen deprivation can also
result in bone problems by
causing a reduction in bone
mineral density. This can
result in osteoporosis,
causing bone pain and an
increased risk of fracture.
From time to time I hear from
men whose first realisation
that this is a possibility is
when they have to attend the
Accident and Emergency
Department of their hospital
following a fracture. It seems
likely to me that as men may
live for many years requiring
hormone therapy, the number of
men developing fractures as a
result of androgen depletion
is likely to increase over the
coming years. It seems
relevant, therefore to try to
prevent this problem
occurring, rather than dealing
with osteoporosis and
fractures. In order to do this
we, and our doctors need to
become proactive in this
area.
There are tests that can
measure levels of bone
density, and apart from
placing an additional burden
on NHS resources (and this is
a very relevant factor that
must be brought into the
debate) I can see no reason
for not performing a
bone-mineral density test to
give a baseline, before men
start on hormone therapy. This
could be followed by periodic
follow up tests.
Oseoclasts and
osteoblasts
It is difficult to discuss
bone integrity without giving
some basic information about
the processes that are
relevant to the structure of
bone. However, I will try not
to be too technical about
it.
Bone is essentially a
latticework of collagen
fibrils that are mineralised.
Osteclasts are cells that
attach themselves to the bone
and excrete acids and
digestive enzymes, which erode
the bone. This process is
called resorption. Androgens
and oestrogens inhibit
osteoclasts and also stimulate
bone-forming cells, known as
osteoblasts. A reduction in
androgens (essentially male
hormones) and oestrogens
(essentially female hormones)
causes an increase in the
population of osteoclasts,
resulting in an increase in
bone resorption
The purpose of osteblasts is
to migrate to areas of bone
that have been eroded by
osteoclasts, and lay down
minerals and collagen in the
cavities that have been left.
This process of osteoclast and
osteoblast activity is
essential for remodelling our
skeleton as changes become
necessary. The problem occurs
when osteoclastic and
osteoblastic activity becomes
excessive, either from cancer
activity, Paget's disease, or
hormone alteration such as
that which occurs with hormone
therapy resulting in androgen
deprivation. We then get into
a vicious circle.
Cancer cells survive by
producing products that
stimulate self-growth. (For
those who wish to know this is
referred to as autocrine
loops) or by producing
proteins or enzymes that
affect nearby cells (paracrine
loops) such as osteoblasts.
Osteoblastic growth requires
calcium and causes a reduction
in serum calcium. This
reduction stimulates
osteoclastic resorption in
order to maintain serum
calcium. The process of
attempting to re-establish the
balance of serum calcium also
requires an increase in a
hormone called parathormone
(PTH) and vitamin D
levels.
Osteoclastic activity
releases certain growth
factors such as Insulin growth
factor-1 (IGF-1) and
transforming growth
factor-beta (TGF-beta). These
stimulate the growth of the
cancer cell population, which
in turn release more insulin
growth factors and proteins,
as well as interluken-1
(IL-1). Together these
stimulate the osteoblasts to
produce interluken-6 (IL-).
IL-6 stimulates more
osteoclasts and osteoclast
precursors.
Overproduction of osteoclasts
results in resorption of bone,
which in turn causes an
increase in osteoblastic
activity. Thus, we get an
increase in bone formation,
but also an increase in bone
resorption. Significantly, new
bone resorption and formation
can take place at different
sites. The bone formation
therefore does nothing to
contribute to bone
strength.
How can we interrupt this
process?
An exciting contributor in
the interruption of this
process is likely to be a
class of drugs called
bisphosphenate. (Remember that
name - you will hear a lot
about it over the next few
months and years).
Bisphosphenates are not new.
They have been around for 30
years. They work by inhibiting
osteoclastic activity and are
often used to treat
osteoporosis and
Paget's Disease. I believe
that in the not too distant
future they will have an
increasing role to play in
metatstic prostate cancer
(cancer that has spread beyond
the prostate gland) and for
treating cancer-induced
hypocalcaemia. Bisphosphenates
have been shown to work at the
tissue, cellular and molecular
level. By that I mean they
decrease bone turnover, by
reducing bone resorption. They
inhibit osteoclastic activity
to the bone surface, thus
shortening the life span of
osteoclasts. At the molecular
level, bisphosphenates inhibit
essential components such as
squalene synthatase and
protein tyrosine
phosphatase.
Put simply, bisphosphenates
appear to:
· Cause cell death
(apoptosis) of osteoclasts
· Interferes with
osteoclastic precursor
cells
· Interferes with the
adhesion of osteoclasts to the
bone matrix
· Interferes with the
adhesion of cancer cells to
the bone matrix - but only
amino bisphosphenates do
this.
Zoledronic acid
(Zoledronate)
Since bisphosphonates were
first introduced 30 years ago,
there have been 3 generations
of the drug. Clodronate is
classed as first generation.
Pamidronate (Aredia) and
Alendronate (Fosamax) are
second generation. Now enters
the third, and possibly most
exciting generation. These
include Ibandrinate and
Zoledronate. Like
second-generation
bisphosphonates, they are
amino- bisphosphonates, but
are many times more potent.
Zoledronate, for example, has
a relative potency (RP) of
1000 compared to Clodronate,
which has an RP of 1. Fosamax
has an RP of 100, and
Ibandronate has an RP of
500.
Zoledronate is made by a
Swiss pharmaceutical company
called Novartis, and is sold
under the name of Zometa. It
is given by intravenous
injection and is being
'fast-tracked' by the USA Food
and Drug Administration (FDA).
This indicates recognition by
the FDA that Zometa may
provide a significant
improvement over existing
drugs. A similar submission
was made to the EMEA in the
European Union on the 30th
July 2001.
The fact that Zometa is given
by intravenous injection may
also be an important factor to
consider. Oral administration
has proved
difficult with
gastrointestinal absorption,
which is said to be about 2%.
An interesting suggestion by
Alfredo Berruti et al is that
for a successful response,
high doses of a potent
bisphosphenate should be given
intravenously, initially,
followed by intravenous or
oral administration at levels
sufficient to maintain
suppressed bone
resorption.
Is there a down side?
Like all treatments for
prostate cancer, there are
potential difficulties
connected with the
administration of
bisphosphonates that also need
to be considered. It has been
suggested that bisphosphonates
do not affect osteoblastic
activity, and that a
persistently high rate of bone
formation may result in
hypocalcaemia and the chronic
stimulation of parathyroid
hormone secretion. If high
levels of parathyroid persist
for a long time, it could
impair the mineralisation of
newly formed bone. Some
researchers have suggested,
however, that patients with
prostate cancer who are being
treated with bisposphenates
should also be given a
supplement of calcium during
treatment to prevent this
response.
A further possibility is that
of an acute phase response,
which is often associated with
fever within 28-36 hours of
the initial injection. A
doctor I know in the USA, Dr
Steven Strum, who uses Aredia
counters this by giving the
first dose of 30 milligrammes
over a period of one and a
half hours. He then increases
the dose to between 60 -90
milligrammes every 2 weeks
thereafter. He has seen 2
cases of kidney damage after
an initial high dose, and says
that this is another good
reason for giving a lower
initial dose.
Trials in the UK
The Prostate Cancer Working
Party, that is part of the
Medical Research Council are
engaged in 4 separate trials
using oral clodronate and
zoledronic acid.
300 participants will be
involved in a multi-centre
double blind randomised trial
to see whether oral sodium
clodronate prolongs the time
for relapse in patients on
hormone therapy for
established bone
metastasis.
In the second trial sponsored
by Novartis, zoledronic acid
is being compared to a placebo
in more than 600 men with
prostate cancer and a history
of bone metastasis and
increasing PSA levels, despite
hormone therapy. The
object is to assess
zoledronic acid for preventing
fractures, spinal chord
compression, surgery to bone
and radiation. It will also
assess tumour and bone
response on bone scan, disease
progression, tolerability and
safety.
The third trial involves 500
men without bone metastasis
and compares the use of oral
clodronate plus hormone
therapy, with men who are
using hormone therapy
only.
Additionally 520 men who are
apparently free from bone
involvement, but have a rising
PSA during hormone therapy,
are being randomised to
intravenous zoledronate
compared to men using a
placebo.
At the moment published data
is insufficient to make a
definitive statement about the
efficacy of bisphosphonates.
Pre-clinical data, however,
strongly suggests that bone
disease that is related to
prostate cancer can benefit
from drugs that inhibit
osteoclastic activity.
Bisphosphonates appear to be
the most effective drug for
doing just that.
Vitamin D3
In 1993 Dr Charles 'Snuffy'
Myers reviewed vitamin D3 in
the area of bone integrity. He
found that research suggests
that synthetic vitamin D3
(Rocaltrol, or Calcitriol) can
enhance calcium absorption
from the gastrointestinal
tract. He also reports that
Rocaltrol has
anti-proliferative and
anti-angiogenisis effects on
prostate cancer growth, and is
able to slow the rate of PSA
rise in men with early
recurrent prostate cancer.
(Anti-angiogenesis means that
it makes it more difficult for
the cancer cells to form
healthy blood vessels. Cancer
cells need a good supply of
blood in order to develop.) He
suggests that it may cause an
increase in urinary excretion
of calcium, but that calcium
supplements taken at night, as
well as a bisphosphonate would
drive the calcium into the
bone and decrease the amount
excreted. He suggests that
synthetic vitamin D3 should
also be taken at bedtime, to
decrease urinary calcium
excretion.
Gren Oades is also carrying
out research into the effects
of vitamin D at St George's
Hospital, London. He makes the
point, as did Gary Schwartz in
1990, that death from prostate
cancer is higher in North
America, where there is less
sunlight, than in the
south.
As we age we are likely to
have lower circulating levels
of vitamin D. Gren Oades also
hypothesises that this may
offer a partial explanation
for the increased risk of
African- American men
developing prostate cancer, as
a result of their darker skin
pigmentation impairing vitamin
D synthesis. If this is true,
it is highly likely that
synthetic vitamin D may offer
some protection to
African-Caribbean men living
in the UK.
It seems that the treatment
of men who have prostate
cancer could be enhanced by
careful and regular thought to
the integrity of bone,
particularly those men who
have metastatic spread to the
bone, or are on androgen
deprivation. It would appear
appropriate, therefore that a
debate about this area of
treatment begins in earnest
immediately.
* I would like to thank my
friends in the USA, Dr Charles
'Snuffy' Myers, Dr Steven
Strum and Roy Bradbrooke for
providing much help and
information for this
article.
References:
Steven Strum. PCRI Insights
(Prostate Cancer Research
Institute) January 1999.
volume 2:1
DE. Hughes et al
'Bisphosphonates promote
apoptosis in murine
osteoclasts in vitro and
vivo'. Journal of Bone Mineral
Res. 10. 1478-1487. 1995
Berruti et al. 'Metabolic
bone disease induced by
prostate cancer: Rationale for
the use of bisphosphonates'.
Journal of Urology, 166;
2023-2031. December 2001
Charles Myers. 'The Prostate
Forum' January 1999
Gren Oades. Update (Prostate
Research Campaign UK) October
2001
Roy Nixon
January 2002
Please note that the
late Roy Nixon wrote as a
prostate cancer patient, not
as a health professional. This
article is intended to
stimulate debate between
patients and doctors and also
between health professionals,
rather than provide medical
advice .All information has
been checked as thoroughly as
possible, but discussion with
health professionals should
always take place before
taking or stopping any
medication.
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