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Their parents call
them “butterfly children,” but
though the words conjure up a sense of poetry and whimsy,
the reality is in harsh contrast. These are children whose
every step is an act of blistering pain, whose skin is so
fragile that it can fall off in shreds within moments after
a parent picks them up. Doctors liken them to burn victims:
their wounds require daily salves, gauze and bandages. Like
burn victims, they need huge numbers of calories to aid in
healing. The more severe among them often are afflicted inside
their mouths as well as on their skin: the disease makes
their teeth fall out, and blisters and scars the esophagus,
making it painful to eat and hard to swallow.
Recessive dystrophic epidermolysis bullosa, or RDEB, is
one of the rarest of genetic skin disorders, a true orphan
disease that afflicts fewer than 500 people in the United
States. And yet—as with many orphan diseases—its
secrets, once unlocked, yield medical clues to some of the
most common conditions. In this case: skin cancer.
“Nature shows us her mysteries through her errors,” says
dermatology professor Paul Khavari. “When you have
a genetic error that leads to disease, it has a lot to
teach you.”
Khavari, ’84, PhD ’94, is one
of 15 or so Stanford scientists converging on the research
and treatment of EB (literally, the breakdown and blistering
of the epidermis; RDEB is one type), with the additional
goal of using it as a gateway to a greater understanding
of skin cancer.
As it happens, Stanford is a national leader
in the field. Its EB clinic employs a multidisciplinary
team of dermatologists, gastroenterologists, nutritionists,
geneticists and oncologists. Together, they diagnose, evaluate
and oversee the treatment of several dozen patients a year.
Although some of those with RDEB live into their 30s, most
succumb to an aggressive form of squamous cell carcinoma.
It is this terrible fate that appears to offer an important
key about one of the most common skin cancers. Squamous
cell, with more than 250,000 new cases reported in the
United States each year, is not, typically, a deadly disease.
Khavari’s early research suggested that it turns
deadly due to the presence of Type VII collagen, a protein
that acts as a glue, anchoring the outer layer of skin to
the inner layer and creating a necessary ingredient to the
spread of skin cancer. RDEB patients have either an altered
version of collagen VII, or a complete absence of the protein.
In 2005, Khavari demonstrated that he could trigger squamous
cell carcinoma in sloughed-off skin samples from children
with RDEB who had a fragment of Type VII collagen, but
not in those that lacked the protein entirely.
Newly published
studies suggest that the involvement of Type VII collagen
in squamous cell may be more complex than first thought.
But that doesn’t seem to disappoint
Khavari. “The truth is beautiful,” he says. “God
forbid we should sit on a lie.”
These days, Khavari
has turned his attention to gene therapy. (He triggered
squamous cell carcinoma in the 2005 study by flipping the
switch on two genes.) Gene therapy is particularly well
suited to treating skin diseases, mostly because skin—the
largest organ in the human body—is much more accessible
than internal organs. In 2002, Khavari successfully performed
gene therapy on human skin grafted onto immunodeficient
mice.
Khavari and associate professor of dermatology M.
Peter Marinkovich are building on this work to transfer
new genes into the intact skin of living patients. They
are applying to the Food and Drug Administration for approval
to begin gene therapy on children with RDEB within the
next year. “We’re
finally
at the stage where we expect to have it in the clinic,” says
Marinkovich, who’s been working on EB research for
the past 16 years.
This is how they do it:
“We take skin cells and introduce normal collagen
Type VII, grow them up a little, then graft the cells back
onto the patients in one of their blistered areas. Then,
we’ll evaluate how long those grafts last. We expect
them to last a long time. Maybe permanently.”
Their
work could lead to advancements in vaccine delivery—imagine
a doctor inoculating your child by dabbing his wrist—and
treatments for other skin disorders. Marinkovich cautions
that gene therapy for skin cancer is a long way away: “It
doesn’t hinge on the success or failure of our gene
therapy.
“The challenge right now is the delivery of the gene.
The magic bullet is to inject the gene into the body and
have it delivered to all the different cells where they’re
required. We’re not there yet.”
When University
dermatologists offered free skin cancer screening at Community
Day in April, 15 percent of the 200 or so people who took
advantage of the offer learned that they did, in fact,
have either a squamous cell or basal cell cancer. In Caucasians,
basal cell carcinoma is, by far, the most common of cancers, numbering
about 900,000 new cases a year.
“It’s scary,” concedes Sabine Kohler,
a professor of dermatology and pathology who is considered
one of the most respected experts in her field. (The two
disciplines have spawned a new specialty, called dermatopathology.) “But
by and large, it’s not that big a deal. You take it
out and you’re done with it. It’s very, very
treatable.”
Far rarer, melanoma—the most deadly
of skin cancers—is
growing at an alarming rate. The National Cancer Institute
reports an increase of 619 percent in melanoma between
1950 and 2000, with a corresponding rise in mortality of
165 percent.
In 2007, an estimated 59,940 Americans will
receive a diagnosis of melanoma; 8,110 will die from the
disease. Many of the new cases will be in young women;
melanoma is the most common cancer among women 20 to 29
years old. A disproportionate number of these will come
from California; the aptly and prophetically named Golden
State has the highest incidence of melanoma in the country.
In 2003, it reported 5,200 new cases.
Although more and
better screening is picking up some of the cases, most
experts agree that the increase is genuine. One in 1,500
Americans born in 1935 had a risk of developing melanoma;
for people born in 2007, the risk is one in 60.
“Melanoma is the only preventable cancer that’s
growing and where the mortality rate is actually increasing,” says
Susan Swetter, associate professor of dermatology and director
of Stanford’s Pigmented Lesion & Cutaneous Melanoma
Clinic. “This is believed to be due to increased ultraviolet
radiation reaching the Earth’s surface as well as
increased sun exposure through outdoor and indoor tanning,
and occupational and recreational activities.”
Swetter
has been studying the sociology of melanoma. She is part
of a national, multicenter study looking at the role wives
and girlfriends of older men play in alerting their partners—the
very ones most at risk of dying from the disease—to
the presence of an “ugly
duckling,” a mole on the back, perhaps, that no one
else may ever see, one whose shape or color has suddenly
begun to morph or grow.
“Where we’re missing the boat, when you look
at the mortality rate, is in these older men,” says
Swetter, referring to studies showing the mortality rate
for men 65 and older grew by 157 percent between 1969 and
1999. “By reaching out to this older male population,
we hope to see how the patterns of discovery took place.
How medical awareness affects treatment, the importance
of social networks, the role that wives play. It’s
going to be an important means of changing our educational
outreach.”
Swetter also is studying the dirty little
secret of melanoma in the United States: the fact that
it is grossly underreported, by as much as 35 percent,
according to one recent survey in Southern California. Despite
federal regulations requiring that all cases of melanoma
be reported to a national registry, many dermatologists
don’t
heed that mandate.
That’s because they can effectively
diagnose and treat thin melanomas—those malignancies
that measure 1 mm or less in thickness—almost entirely
in their offices, explains Swetter, who is working with
the California Cancer Registry on a study of dermatologists
in the Bay Area.
If melanoma is caught early, patients have an excellent
prognosis. “The beauty of melanoma is that it’s
right there to see,” says Kohler. “So there’s
an excellent chance of recognition and treatment—as
opposed to pancreatic cancer, where the patient doesn’t
have symptoms until very late. Melanoma is right out there.”
A dermatologist can walk into an examining room and, with
90 percent accuracy, diagnose a lesion as a mole, basal
cell carcinoma, squamous cell carcinoma or melanoma. That
degree of precision drops below 60 percent for doctors
and other health professionals untrained in dermatology.
Most cases of melanoma are still in the thin stage when
diagnosed. A tumor that is less than 1 mm thick is less
likely to have metastasized into the lymph nodes, at which
stage it becomes far more deadly.
But 15 percent of melanomas
less than 1 mm ultimately metastasize, while some patients
with thick melanomas will live and thrive. Soheil Sam Dadras,
a young dermatopathologist, is frustrated by the lack of
accurate prognosis. Breslow Depth has been the standard
for decades, used by dermatopathologists to measure how
thick a melanoma is from top to bottom. They use the results,
along with the Clark Level, which interprets skin thickness,
to determine severity and prognosis of the cancer.
“It’s inconclusive,” the assistant professor
says. “I just saw a 24-year old woman who has a very
thin melanoma on her calf, which is the most common place
for women to get it. She’s already developed a metastasis
in her lymph nodes and I don’t think she’s going
to do well.
“There’s a big problem understanding which
melanomas are going to act badly. So I’m trying to
develop the Stanford Melanoma Index. It’s based on
tumor thickness, how rapidly the cells divide, and the number
of lymphatic vessels that are involved,” Dadras says. “The
idea is that this index will predict how patients with
melanoma will fare.”
He is planning to work with Swetter
and Andrew Fire, the molecular geneticist who last year
won the Nobel Prize for his discovery of how double-stranded
RNA can switch off genes one at a time.
Dadras has chosen
not to work with animal models, partly because they’re
so expensive (a genetically engineered mouse colony can
run between $30,000 and $40,000 a year), partly because
mice simply make poor hosts for studying melanoma. Mice
are nocturnal animals; even after being given the disease,
they never go on to actually develop lymphatic, systemwide
cancer. In other words, melanoma can’t
kill a mouse.
So Dadras plans to tackle the disease in
humans—by
going back to the stacks, the warehouses storing hundreds
of thousands of small paraffin blocks with human archival
tissues from biopsies done at Stanford Hospital over the
past 30 years. They look like little pieces of sandy meat
embedded in wax, but to Dadras they represent a gold mine.
“Tumor samples,” says Dadras. “That’s
where we hope to make a difference. I’m starting with
actual human disease. Fresh frozen melanoma is very difficult
to find, because we need most of the lesion to make the
diagnosis. But we’re trying to change that. I’m
working with Denise Johnson, our melanoma surgeon, and
hopefully a couple others, to get
more material.
“If we can extract RNA from the paraffin blocks and
then follow these patients and see how [the tissue samples]
correlated with clinical behavior, we might see a pattern
that tells us about how it metastasizes. My goal is to
make it simple, easy and reproducible so that it can be
available as a clinical test.
“Melanoma is one of the least understood of all tumors,” he
continues. “If you think about a lung tumor, it can
grow from the size of a golf ball to literally the size
of a melon. Melanoma is small by comparison.”
There
aren’t a lot of effective treatments for metastatic
melanoma. A personalized cancer vaccine showed some early
promise in extending survival for late-stage melanoma patients,
but the results have ultimately disappointed.
There is new
hope that that may change. In May, a small study by associate
professor Peter Lee, a hematologist whose research focuses
on the biology of immune response to cancer, shed new light
on why the human immune system isn’t
able to stop melanoma in its tracks.
Lee’s group found
that the immune cells in most people with melanoma fail
to respond to interferon, the molecule that normally activates
the immune system. Without the ability to respond to interferon,
the cells are less able to fend off the cancer.
Lee’s
study has been cited as the first real explanation behind
a decade of research showing that people with cancer often
have dysfunctional immune systems. Finding the disruption
in the cancer cells’ interferon response may help
in the development of vaccines to treat cancers.
A number
of interventions already exist for squamous and basal
cell carcinoma. But surgery—the gold standard—can
be disfiguring to patients with multiple lesions. Stanford
researchers have conducted early studies that suggest cosmetic
treatments for wrinkles, such as laser facial resurfacing,
chemical peels and topical creams, could be beneficial.
These treatments resulted in an 83 percent to 92 percent
decrease in actinic keratoses, rough patches of skin that
appear on sun-exposed areas and are considered precursors
to cancer. All, according to a 2006 Stanford study, may
reduce precancerous lesions and lower the risk of skin
cancer.
If the spa treatments don’t pan out, there’s
always the Rogaine-style solution. Associate professor
of dermatology Anthony Oro and colleagues are at work on
additional topical treatments for basal cell, partly inspired
by his work on hair regeneration. “These basal cell
carcinomas are basically hair cells that try to make a
hair and keep growing,” Oro explains.
Like several
brain tumors, basal cell carcinoma carries a mutation in
a signaling pathway called hedgehog—so
called because it resembles a protein in the fruit fly
gene that looks like a hedgehog.
“There’s a group of us working on it at Stanford,” says
Oro, ’85. “It has given us some very interesting
leads—both how to kill the tumor by blocking the pathway
and changing the ‘soil’ in which it grows, as
well as stopping the growth signals in the tissue around
it.”
The study of basal cell carcinoma is rich because
of its relationship to other, more lethal cancers. To understand
why, Oro says, think of the skin as a sheet of cells—much
like the lung, gut and intestine.
“It’s surprising, but it’s really quite
similar to the way the lungs and pancreas develop,” says
Oro. “They don’t look the same, but they have
very common strategies in the ways they develop and are
maintained.”
“At first it seems so different,” says Howard
Chang, an assistant professor of dermatology whose lab
has been studying the phenomenon of wound healing. “But
it turns out the same genes and same pathways are used
in different organs and what you learn from one is useful
in learning about another.”
As a wound heals, hitherto
inactive cells respond and move into position, bypassing
the normal rules of biologic behavior to begin the work
of repairing the body. When cancer metastasizes, it takes
advantage of that same repair process and usurps it to
its own end. Which is why Chang describes cancer as a wound
gone wild.
In many cases, cancer even looks like healing
tissue—while
never ultimately healing. In fact, Chang notes, a chronic
ulcer or wound can actually turn cancerous.
The best example
of that, he says, is a little-known disease characterized
by wounds: RDEB.
“You might think you want to understand one problem,” Chang
says, “but it turns out that by understanding research
in general, the rare disease shows you some aspect of biology
in a spectacular way. |
