This
is a long post about clinical trials and my experience so far. Not for everyone.
What
is a clinical trial? A clinical trial is a research study done
after previous research (typically in animals) has shown that a new compound or
treatment may be beneficial to patients.
Trials are typically funded and managed by the company or institution
that created the treatment; however, in some cases the government will fund a
study through, for example, the National Institute of Health (NIH). The NIH describes clinical trials this way:
· Phase I: Researchers test a new
drug or treatment in a small group of people for the first time to evaluate its
safety, determine a safe dosage range, and identify side effects.
· Phase II: The drug or treatment
is given to a larger group of people to see if it is effective and to further
evaluate its safety.
· Phase III: The drug or treatment
is given to large groups of people to confirm its effectiveness, monitor side
effects, compare it to commonly used treatments, and collect information that
will allow the drug or treatment to be used safely.
·
Phase IV: Studies are done after
the drug or treatment has been marketed to gather information on the drug's
effect in various populations and any side effects associated with long-term
use.
I
think a Phase I trial may be the most dangerous and unpleasant of the trials
because before the trial, the researchers do not really know how people will
respond to the treatment. Part of the
trial is a dose escalation phase in which the maximum tolerable dose is
determined. Patients are given
increasingly stronger doses until they develop serious side effects or quit the
trial because of the side effects. My
clinical trial is an expansion of Phase I.
The drug GDC-0919 has been given to a small number of patients and the
effects of different dose levels have been examined. The expansion adds additional patients with
different cancers and different characteristics. I think it may be unusual, but my trial is
being conducted at 11 sites in the US and is being set up in three sites each
in France, Korea, and Spain. It suggests
to me that they think they are on to something good with GDC-0919.
A
Phase I trial also provides some evidence of effectiveness; however, more patients
with perhaps different diseases are needed to get sufficient evidence of
success, the Phase II trial.
The
Phase III trial is where the rubber meets the road. In this phase, the new treatment is compared
with a previously approved drug or treatment to measure effectiveness and
safety. I think Phase III trials are
often done in multiple locations in order to get more and a better variety of
patients. If the Phase III trial shows
that the treatment is effective, the sponsor determines whether or not to seek
approval from the Food and Drug Administration (in the US).
How does one find
clinical trials? A clinical trial may be suggested by your
doctor, or you can go online and search for them. The best source of trials can be found on the
NIH website: https://clinicaltrials.gov/. You can search by disease and trial
location. If you look at the entry for
my trial (https://clinicaltrials.gov/ct2/show/NCT02471846?term=gdc-0919&rank=1) you will see:
· the purposes of the study,
· a description of the various arms (groups of patients) of the study,
· the requirements for participation in the study,
· the conditions for elimination for the study, and
· information about where the study is being conducted.
If
you live near a NCI designated Comprehensive Cancer
Center,
you can probably find a list of locally available trials on their web site.
How to join a trial. When I applied for a clinical trial run by
the NCI last January, I think I applied before talking to my oncologist about
it; however, I think it would be a good idea to talk to your doctor first. You first contact the study coordinator and
complete their paperwork. I had to have
the hospital send certain medical records to the NCI. For the trial here in Denver the hospital
already had the medical records on hand.
The
medical records are used to determine if you are sick enough but not too sick
to participate in the trial. They look
at the list of inclusion criteria to ensure that you are sick enough. For example, in my case, I had to have solid
tumors, and they had to show “Progression following at
least one standard therapy; or standard therapy considered ineffective,
intolerable, or inappropriate; or use of an investigational agent recognized as
a standard of care.” The idea being that
they do not want to use an experimental drug that might be unsuccessful when an
already approved standard treatment is available.
They
also want to make sure that participants do not have other conditions that
might keep them from completing the trial.
The NCI rejected my application because I use supplemental oxygen; i.e.
I was too sick to participate. I asked
my oncologist to let them know that I lived in mile-high Denver and had not
used oxygen the summer before when traveling from Denver to Michigan and back. Bethesda, MD is near sea level, so I would be
OK. They accepted his argument, and I
was accepted; however, congestive heart failure arose, and I withdrew from the
trial.
The prescreening. For my trial, I had to have a prescreening
visit in which I was weighed, measured, and poked. I also had to have a tumor biopsy because my
tumor cells had to display the PD-L1 protein.
That involved inserting a coring needle through my back into my tumor
and extracting a piece of the tumor. The
procedure was done as a day-surgery, and I was given some anesthesia during the
process. Of course, you have to go
through a consent form with the provider to ensure that you know what will be
happening and what the risks are. My consent
form was eight pages long, but it was clear and the nurse practitioner made
sure we talked about all aspects of the form.
Starting the Trial. A week before my first treatment, I had
another exam, many tubes of blood drawn, and a CT of my lungs. Genentec, the company sponsoring the trial,
covers the bases thoroughly. Eighteen
blood tests were run on the blood drawn that day. The consent form was 37 pages long, but the
nurse practitioner went over it page by page to make sure everything was
clear. To participate, you basically
give your body to them. I agreed . . .
· that I would receive no compensation for participation,
· that they can take the tissue as described in the consent form,
· that they can keep what is in excess for other research purposes, and
· that I understood that the risks of the treatment are not fully
understood because it is experimental.
They
agreed . . .
· that I can withdraw from the program at any time,
· that they will bear the costs of the study including treatment for harm
done by the treatment,
· that I am responsible for any costs that would be part of my regular
medical treatment, and
· that they will protect my privacy.
The study is run in three-week cycles, and the consent form went through what would be done in each cycle—blood draws, infusions, CTs, biopsies, etc.
For Genentec this is more than a study of how
effective these two drugs, Tecentriq and GDC-0919, are when given together and
how they might interact. The tissue and
blood samples will contribute to their ongoing research about how cancer forms
and spreads. They may sequence my entire
genome for their research purposes, and neither I nor my doctor will have
access to the results. They may make
tons of money from the combined data of the participants. I’m OK with that because my cells and
molecules might contribute to the advancement of science and medicine. I’m happy to contribute in honor of the
clinical trial participants who paid it forward in getting us to the state we
are in now with cancer treatment.
One
week later, October 27, when all that information had be examined, I went to
the hospital for my first treatment.
More routine blood draws and a urinalysis were performed, and when the
results didn’t find any problems, I went down to the infusion center to get my
first dose of Tecentriq. The infusion
took 30 minutes, and I had to wait under observation for 30 more minutes with a
blood draw before the infusion and after the observation period. Nothing happened to be observed.
Blood
is taken at different times in a trial cycle for three purposes. General blood tests and a urinalysis are
taken before any office visit to see if my general health is strong enough to
continue. At an infusion of Tecentriq or
the initiation of a new round of GDC-0910, they take pharmacokinetic blood
samples to see how long the drug remains in my body and pharmacodynamic (PD) samples
to see how the body processes the drug at the same time.
I had a long day at the hospital when I returned
almost three weeks later for a Tecentriq infusion and my first dose of
GDC-0919. I had a blood draw at 7:10 am,
a visit with my oncologist at 8:15 am, and then went down to the infusion
center. I finally left the hospital
about 5:45 pm. They took blood before
and after my infusion. After taking my
first dose of GDC-0919 they took blood at 15 minutes, 30 minutes, 1, 2, 4, 6,
and 8 hours after dosing. About a cup of
blood is taken in total on these long days.
When I go back tomorrow for the start of my second cycle of the oral
drug, I’ll have another long day, but that is the last one. After that the blood draws will only be taken
before treatment.
I have a port implanted under the skin of my chest
which is connected by a tube to a large blood vessel, the superior vena
cava. It is accessed (virtually
painlessly) when I go the lab at the start of a day. I am left accessed which means that a sort of
pigtail of tubing comes from the port needle and is used throughout the day to
take blood. The needle is removed at the
end of the day (painlessly). I love my
port; however, when I get an infusion they cannot draw blood from the port
because of concern that all the drug would not be flushed out and would
contaminate the blood draw. On those
days, I get an IV for the infusion, and all of the blood draws are taken from
the port.
So what do I do on those long days? Once they get through the first few blood
draws, I am moved from the infusion chair to a room with recliners where
subsequent blood draws are taken. I can
leave and go downstairs to eat, walk around, etc. as long as I am back in the
room for my next scheduled blood draw.
Last week I read a book, a magazine, and the news on the internet and
played Spider Solitaire. By the way, the
people in the infusion center are great—friendly, helpful, smart,
knowledgeable, efficient, and on top of things.
I am always inspired by the competence of the people at the University
of Colorado Hospital.