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What is cancer?
Cancer develops when cells in a part of the body begin to grow
out of control. Even though there are many kinds of cancer, they all
start because of abnormal cells that grow out of control.
Normal body cells grow, divide, and die in an orderly fashion.
During the early years of a person's life, normal cells divide more
rapidly until the person becomes an adult. After that, cells in most
parts of the body divide only to replace worn-out or dying cells and to
repair injuries.
Because cancer cells continue to grow and divide, they are
different from normal cells. Instead of dying, they outlive normal
cells and continue to form new abnormal cells.
Cancer cells often travel to other parts of the body where
they begin to grow and replace normal tissue. This process, called
metastasis, occurs as the cancer cells get into the bloodstream or
lymph vessels of our body. When cells from a cancer like breast cancer
spread to another organ like the liver, the cancer is still called
breast cancer, not liver cancer.
Cancer cells develop because of damage to DNA. This substance
is in every cell and directs all its activities. Most of the time when
DNA becomes damaged the body is able to repair it. In cancer cells, the
damaged DNA is not repaired. People can inherit damaged DNA, which
accounts for inherited cancers. Many times though, a person’s
DNA becomes damaged by exposure to something in the environment, like
smoking.
Cancer usually forms as a solid tumor. Some cancers, like
leukemia, do not form tumors. Instead, these cancer cells involve the
blood and blood-forming organs and circulate through other tissues
where they grow.
Not all tumors are cancerous. Benign (non-cancerous) tumors do
not spread to other parts of the body (metastasize) and, with very rare
exceptions, are not life threatening.
Different types of cancer can behave very differently. For
example, lung cancer and breast cancer are very different diseases.
They grow at different rates and respond to different treatments. That
is why people with cancer need treatment that is aimed at their
particular kind of cancer.
Cancer is the second leading cause of death in the United
States. Half of all men and one-third of all women in the United States
will develop cancer during their lifetimes. Today, millions of people
are living with cancer or have had cancer. The risk of developing most
types of cancer can be reduced by changes in a person's lifestyle, for
example, by quitting smoking and eating a better diet. The sooner a
cancer is found and treatment begins, the better are the chances for
living for many years.
Oldest descriptions of cancer
Cancer has afflicted humans throughout recorded history. It is
no surprise that from the dawn of history people have written about
cancer. Some of the earliest evidence of cancer is found among
fossilized bone tumors, human mummies in ancient Egypt, and ancient
manuscripts. Bone remains of mummies have revealed growths suggestive
of the bone cancer, osteosarcoma. In other cases, bony skull
destruction as seen in cancer of the head and neck has been found.
Our oldest description of cancer (although the term cancer was
not used) was discovered in Egypt and dates back to approximately 1600
B.C. The Edwin Smith Papyrus, or writing, describes 8 cases of tumors
or ulcers of the breast that were treated by cauterization, with a tool
called "the fire drill." The writing says about the disease, "There is
no treatment."
Origin of the word cancer
The origin of the word cancer is credited to the Greek
physician Hippocrates (460-370 B.C.), considered the "Father of
Medicine." Hippocrates used the terms carcinos and carcinoma to
describe non-ulcer forming and ulcer-forming tumors. In Greek these
words refer to a crab, most likely applied to the disease because the
finger-like spreading projections from a cancer called to mind the
shape of a crab. The Roman physician, Celsus (28-50 B.C.), later
translated the Greek term into cancer,
the Latin word for crab. Galen (130-200 A.D.), another Roman physician,
used the word oncos
(Greek for swelling) to describe tumors. Although the crab analogy of
Hippocrates and Celsus is still used to describe malignant tumors,
Galen's term is now used as a part of the name for cancer specialists
-- oncologists.
Renaissance period
During the Renaissance, beginning in the 15th century,
scientists in Italy developed a greater understanding of the human
body. Scientists such as Galileo and Newton began to use the scientific
method, which later began to be used to study disease. Autopsies,
performed by Harvey (1628), allowed an understanding of the circulation
of blood through the heart and body that had remained a mystery.
In 1761, Giovanni Morgagni of Padua was the first to do
something considered routine today. He performed autopsies to relate
the patient's illness to the pathologic findings after death. This laid
the foundation for scientific oncology, the study of cancer.
The famous Scottish surgeon John Hunter (1728-1793) suggested
that some cancers might be cured by surgery and described how the
surgeon might decide which cancers to operate on. If the tumor had not
invaded nearby tissue and was "moveable," he said, "There is no
impropriety in removing it."
A century later the development of anesthesia allowed surgery
to flourish and the classic cancer operations such as radical
mastectomy were developed.
Nineteenth century
The 19th century saw the birth of scientific oncology with the
discovery and use of the modern microscope. Rudolf Virchow, often
called the founder of cellular pathology, provided the scientific basis
for the modern pathologic study of cancer. As Morgagni had correlated
the autopsy findings observed with the unaided eye with the clinical
course of illness, so Virchow correlated the microscopic pathology.
This method not only allowed a better understanding of the
damage cancer had done to a patient but also laid the foundation for
the development of cancer surgery. Body tissues removed by the surgeon
could now be examined and a precise diagnosis made. In addition, the
pathologist could tell the surgeon whether the operation had completely
removed the tumor.
Cancer causes
From the earliest times, physicians have wondered about the
cause of cancer. The Egyptians blamed cancers on the Gods.
Humoral theory:
Hippocrates believed that the body contained 4 humors (body
fluids) -- blood, phlegm, yellow bile, and black bile. A balance of
these fluids resulted in a state of health. Any excesses or
deficiencies caused disease. An excess of black bile collecting in
various body sites was thought to cause cancer. This theory of cancer
was passed on by the Romans and was embraced by the influential doctor
Galen’s medical teaching, which remained the unchallenged
standard through the Middle Ages for over 1300 years. During this
period, the study of the body, including autopsies, was prohibited for
religious reasons, thus limiting knowledge.
Lymph theory: Among
theories that replaced the humoral theory of cancer was cancer's
formation by another fluid, lymph. Life was believed to consist of
continuous and appropriate movement of the fluid parts through solids.
Of all the fluids, the most important were blood and lymph. Stahl and
Hofman theorized that cancer was composed of fermenting and
degenerating lymph varying in density, acidity, and alkalinity. The
lymph theory gained rapid support. John Hunter (1723-1792) agreed that
tumors grow from lymph constantly thrown out by the blood.
Blastema theory:
In 1838, German pathologist Johannes Muller demonstrated
that cancer is made up of cells and not lymph, but he was of the
opinion that cancer cells did not arise from normal cells. Muller
proposed that cancer cells arose from budding elements (blastema)
between normal tissues. His student, Rudolph Virchow (1821-1902), the
famous German pathologist, determined that all cells, including cancer
cells, are derived from other cells.
Chronic
irritation: Virchow proposed that chronic irritation was
the cause of cancer, but he falsely believed that cancers "spread like
a liquid." A German surgeon, Karl Thiersch, showed that cancers
metastasize through the spread of malignant cells and not through some
unidentified fluid.
Trauma: Despite
advances in the understanding of cancer, from the late 1800s until the
1920s, cancer was thought by some to be caused by trauma. This belief
was maintained despite the failure to cause cancer in experimental
animals by injury.
Parasite theory:
In the 17th and 18th centuries, some believed that cancer was
contagious. In fact, the first cancer hospital in France was forced to
move from the city in 1779 because of the fear of the spread of cancer
throughout the city.
A Nobel Prize was wrongly awarded in 1926 for scientific
research documenting stomach cancer being caused by a certain worm.
Scientists were unable to confirm this research, so they lost interest
in the parasite theory.
By the middle of the 20th century, scientists had in their
hands the instruments needed to begin solving the complex problems of
chemistry and biology presented by cancer. James Watson and Francis
Crick, who received a Nobel Prize in 1962 for their work, had
discovered the exact chemical structure of DNA, the basic material in
genes.
DNA was found to be the basis of the genetic code that gives
orders to all cells. After learning how to translate this code,
scientists were able to understand how genes worked and how they could
be damaged by mutations (changes or mistakes in genes). These modern
techniques of chemistry and biology answered many complex questions
about cancer.
Scientists already knew that cancer could be caused by
chemicals, radiation, and viruses, and that sometimes cancer seemed to
run in families. But as our understanding of DNA and genes increased,
we learned that it was the damage to DNA by chemicals and radiation or
introduction of new DNA sequences by viruses that often led to the
development of cancer. It became possible to pinpoint the exact site of
the damage to a specific gene.
Further, scientists discovered that sometimes defective genes
are inherited and that sometimes these inherited genes are defective at
the same points that chemicals exerted their effect. In other words,
most carcinogens caused genetic damage (mutations), mutations led to
abnormal groups of cells (called clones), mutant clones evolved to even
more malignant clones over time, and the cancer progressed by more and
more genetic damage and mutations. Normal cells with damaged DNA die;
cancer cells with damaged DNA do not. The recent discovery of this
critical difference answers many questions that have troubled
scientists for many years.
During the 1970s, scientists discovered 2 important families
of genes -- oncogenes and tumor suppressor genes.
Oncogenes are
mutated forms of genes that cause normal cells to grow out of control
and become cancer cells. They are mutations of certain normal genes of
the cell called proto-oncogenes. Proto-oncogenes are the genes that
normally control how often a cell divides and the degree to which it
differentiates (or specializes).
Tumor suppressor genes are
normal genes that slow down cell division, repair DNA mistakes, and
tell cells when to die (a process known as apoptosis or programmed cell
death). When tumor suppressor genes don’t work properly,
cells can grow out of control, which can lead to cancer. It may be
helpful to think of a cell as a car. For it to work properly, there
need to be ways to control how fast it goes. A proto-oncogene normally
functions in a way that is similar to a gas pedal -- it helps the cell
grow and divide. An oncogene could be compared to a gas pedal that is
stuck down, which causes the cell to divide out of control. A tumor
suppressor gene is like the brake pedal on a car -- it normally keeps
the cell from dividing too quickly just as a brake keeps a car from
going too fast. When something goes wrong with the gene, such as a
mutation, cell division can get out of control.
Slowly, medical scientists are identifying the oncogenes and
tumor suppressor genes that are damaged by chemicals or radiation and
the genes that, when inherited, can lead to cancer. For example, the
discovery during the 1990s of 2 genes that cause some breast cancers,
BRCA1 and BRCA2, represents considerable promise because many people
who have a higher probability of developing breast cancer can now be
identified
Other genes have been discovered that are associated with some
cancers that run in families, such as cancers of the colon, rectum,
kidney, ovary, thyroid, pancreas and skin melanoma. Familial cancer is
not nearly as common as spontaneous cancer, causing less than 15% of
all cancers, but it is important to understand these cancers because
with continued research in genetics we may be able to identify persons
at very high risk.
Modern day carcinogens
More recently, other causes of cancer were discovered and
documented. In 1911 Peyton Rous, at the Rockefeller Institute in New
York, described a type of cancer (sarcoma) in chickens caused by what
later became known as the Rous sarcoma virus. He was awarded the Nobel
Prize for that work in 1968. In 1915 cancer was induced in laboratory
animals for the first time by a chemical, coal tar, applied to rabbit
skin at Tokyo University. One hundred and fifty years had passed since
the most destructive source of chemical carcinogens known to man,
tobacco, was first identified in London by the astute clinician John
Hill. It was to be many years until tobacco was "rediscovered" as a
carcinogen (a substance known or believed to cause cancer in humans).
Today we recognize and avoid many specific substances that
cause cancer: coal tars and their derivatives such as benzene, some
hydrocarbons, aniline (a substance used to make dyes), asbestos, and
others. Radiation from a variety of sources, including the sun, is
known to lead to cancer. To ensure the public's safety, the government
has set standards for many substances, such as benzene, asbestos,
hydrocarbons in the air, arsenic in drinking water, radiation, and so
on.
Several viruses are now linked to cancer:
- Long-standing liver infection with the hepatitis B or C
viruses can lead to cancer of the liver.
- A variety of the herpes virus, the Epstein-Barr virus,
causes infectious mononucleosis and has been implicated in non-Hodgkin
lymphomas and nasopharyngeal cancer.
- The human immunodeficiency virus (HIV) is associated with
an increased risk of developing several cancers, especially Kaposi
Sarcoma and non-Hodgkin lymphoma.
- Human papilloma viruses (HPVs) have been linked to several
cancers, especially those of the cervix, vulva, and penis. A test for
types HPV types linked to cervical cancer was approved by the FDA for
clinical use in cervical cancer screening in 2003. A vaccine that
prevents infection with 2 cancer-associated HPV types was approved by
the FDA in 2006 for use in cancer prevention.
As of 2008, the World Health Organization's International
Agency for Research on Cancer (IARC) has identified more than 100
chemical, physical, and biological carcinogens. Many of these
associations were recognized long before scientists understood the
mechanism by which the cancer was produced, but continuing research is
discovering new carcinogens, explaining how they cause cancer, and
providing insight into ways to prevent cancer.
Cancer epidemiology
During the 18th century, 3 important observations were made
that launched the field of cancer epidemiology.
- Bernardino Ramazzini, an Italian doctor, reported in 1713
the virtual absence of cervical cancer and relatively high incidence of
breast cancer in nuns and wondered whether this was in some way related
to their celibate lifestyle. This observation was an important step
toward identifying and understanding the importance of hormonal factors
such as pregnancy and infections related to sexual contact in modifying
cancer risk.
- Percival Pott of Saint Bartholomew's Hospital in London
described in 1775 an occupational cancer in chimney sweeps, cancer of
the scrotum, caused by soot collecting under their scrotum. This
research led to many additional studies that identified a number of
occupational carcinogenic exposures and led to public health measures
to reduce cancer risk.
- John Hill of London was the first to recognize the dangers
of tobacco. In 1761, only a few decades after tobacco became popular in
London, he wrote a book entitled Cautions
Against the Immoderate Use of Snuff.
- Results of epidemiologic research published during the
1950s and early 1960s demonstrate that smoking is a cause of lung
cancer, and lead to the US Surgeon General's 1964 report Smoking and
Health.
Epidemiologists continue their search for factors that cause
cancer (such as tobacco use, obesity, ultraviolet radiation) as well as
those offering protection against cancer (such as physical activity,
healthful diet). This research provides evidence to guide pubic health
recommendations and regulations. As molecular biologists learn more
about how factors cause of prevent cancer, this information is used in
studies of molecular epidemiology, which study the interactions between
genes and external factors.
Cancer screening and early detection
Screening refers to tests and exams used to find a disease,
such as cancer, in people who do not have any symptoms. The first
screening test to be widely used for cancer was the Pap test. The test
was first developed by George Papanicolaou as a research method in
understanding the menstrual cycle. Papanicolaou soon recognized its
potential for early detection of cervical cancer and presented his
findings in 1923. Most doctors were initially skeptical, and it was not
until the American Cancer Society promoted the test during the early
1960 that this test was widely used. Since that time, the cervical
cancer death rate in the United States has declined by about 70%.
Modern mammography methods were developed late in the 1960s and first
officially recommended by the ACS in 1976.
Current American Cancer Society guidelines include methods for
early detection of cancers of the cervix, breast, colon and rectum,
endometrium, and prostate, as well as a cancer-related checkup which,
depending on a person's age and gender, might include exams for cancers
of the thyroid, oral cavity, skin, lymph nodes, testes, and ovaries.
Cancer treatments: surgery
Ancient physicians and surgeons knew that cancer would usually
come back after it was removed by surgery. The Roman physician Celsus
wrote, "After excision, even when a scar has formed, none the less the
disease has returned."
Galen was a 2nd-century Roman doctor whose books were
preserved for centuries and who was thought to be the highest medical
authority for over a thousand years. Galen viewed cancer much as
Hippocrates had, and his views set the pattern for cancer management
for centuries. He considered the patient incurable after a diagnosis of
cancer had been made.
Even though medicine progressed and flourished in some ancient
civilizations, there was little progress in cancer treatment. The
approach to cancer was Hippocratic (or Galenic) for the most part. To
some extent this view that cancer cannot be cured has persisted even
into the 20th century. This has served to fuel the fear patients have
of the disease. Some people, even today, consider all cancer incurable
and delay consulting a doctor until it is too late.
Treatments for cancer went through a slow process of
development. The ancients recognized that there was no curative
treatment once a cancer had spread and that intervention might be more
harmful than no treatment at all. Galen did write about surgical cures
for breast cancer if the tumor could be completely removed at an early
stage. Surgery then was very primitive with many complications,
including blood loss. It wasn't until the 19th and early 20th centuries
that major advances were made in general surgery and specifically in
cancer surgery.
There were great surgeons before the discovery of anesthesia.
John Hunter, Astley Cooper, and John Warren achieved lasting acclaim
for their swift and precise surgery. But when anesthesia became
available in 1846, there emerged the great surgeons whose work so
rapidly advanced the art that the next hundred years became known as
"the century of the surgeon."
Three surgeons stand out because of their contributions to the
art and science of cancer surgery: Bilroth in Germany, Handley in
London, and Halsted at Johns Hopkins. Their work led to "cancer
operations" designed to remove all of the tumor together with the lymph
nodes in the region where the tumor was located.
William Stewart Halsted, professor of surgery at Johns Hopkins
University, developed the radical mastectomy during the last decade of
the 19th century. His work was based in part on that of W. Sampson
Handley, the London surgeon who believed that cancer spread outward by
invasion from the original growth.
Halsted did not believe that cancers usually spread through
the bloodstream: "Although it undoubtedly occurs, I am not sure that I
have observed from breast cancer, metastasis which seemed definitely to
have been conveyed by way of the blood vessels." He believed that
adequate local removal of the cancer would be curative -- if the cancer
later appeared elsewhere, it was a new process. That belief led him to
develop the radical mastectomy for breast cancer. This became the basis
of cancer surgery for almost a century until the 1970s, when modern
clinical trials demonstrated that less extensive surgery is equally
effective for most women with breast cancer. Today, the radical
mastectomy is almost never performed and the "modified radical
mastectomy" is performed less frequently than before; most women with
breast cancer undergo local removal of the primary tumor (lumpectomy)
coupled with radiation therapy.
At the same time Halsted and Handley were developing their
radical operations, another surgeon was asking, "What is it that
decides which organs shall suffer in a case of disseminated cancer?"
Stephen Paget, an English surgeon, concluded that cancer cells spread
by way of the bloodstream to all organs of the body but were able to
grow only in a few organs. In a brilliant leap of logic he drew an
analogy between cancer metastasis and seeds that "are carried in all
directions, but they can only live and grow if they fall on congenial
soil."
Paget's conclusion that cells from a primary tumor spread
through the bloodstream but could grow only in certain, and not all,
organs was an accurate and highly sophisticated hypothesis that was
confirmed by the techniques of modern cellular and molecular biology
almost a hundred years later. This understanding of metastasis became a
key element in recognizing the limitations of cancer surgery. It
eventually allowed doctors to develop systemic treatments used after
surgery to destroy cells that had spread throughout the body and to use
less mutilating operations, for example, in treating many types of
cancer. Today these systemic treatments may also be used before
surgery.
During the final decades of the twentieth century, surgeons
developed greater technical expertise in minimizing the amounts of
normal tissue removed during cancer operations. Like the trend from
radical mastectomy to lumpectomy, progress was also made in removing
bone and soft tissue tumors of the arms and legs without the need for
amputation in most cases, and in avoiding a colostomy for most patients
with rectal cancer. This progress depended not only on better
understanding of cancer as a disease and on better surgical
instruments, but also on combining surgery with chemotherapy and/or
radiation.
Until the end of the twentieth century, cancer diagnosis
required "exploratory surgery" to open the abdomen or chest so the
surgeon could take tissue samples to be tested for cancer. Starting in
the 1970s, progress in ultrasound (sonography), computed tomography (CT
scans), magnetic resonance imaging (MRI scans), and positron emission
tomography (PET scans) have replaced most exploratory operations. CT
scans and ultrasound can be used to guide biopsy needles into tumors of
internal organs.
Instruments that use fiberoptic technology and miniature video
cameras permit doctors to view the inside of the body. Surgeons can use
special surgical instruments operated through tubes inserted into the
body. Endoscopic surgery can remove tumors through tubes inserted
through body openings to reach the colon, esophagus, or bladder.
Similar instruments can also be inserted through small incisions to
reach the abdomen (laporscopic surgery) or chest (thorascopic surgery).
Less invasive ways of destroying tumors without removing them
are being studied and/or used. Cryosurgery (also called cryotherapy or
cryoablation) uses liquid nitrogen spray or a very cold probe to freeze
and kill abnormal cells. Lasers can be used to cut through tissue
(instead of using a scalpel) or to vaporize (burn and destroy) cancers
of the cervix, larynx (voice box), liver, rectum, skin and other
organs. Radiofrequency ablation transmits radio waves to a small
antenna placed in the tumor to kill cancer cells by heating them.
Cancer treatments: hormone therapy
Another 19th-century discovery laid the groundwork for an
important modern method to treat and prevent breast cancer. Thomas
Beatson graduated from the University of Edinburgh in 1874 and
developed an interest in the relation of the ovaries to milk formation
in the breasts, probably because he grew up near a large sheep farm in
rural Scotland. In 1878 he discovered that the breasts of rabbits
stopped producing milk after he removed the ovaries. He described his
results to the Edinburgh Medico-Chirurgical Society in 1896: "This fact
seemed to me of great interest, for it pointed to one organ holding
control over the secretion of another and separate organ."
Because the breast was "held in control" by the ovaries,
Beatson decided to test removal of the ovaries (oophorectomy) in
advanced breast cancer. He found that oophorectomy often resulted in
the improvement of breast cancer patients. He also suspected that "the
ovaries may be the exciting cause of carcinoma" of the breast. He had
discovered the stimulating effect of the female ovarian hormone
(estrogen) on breast cancer, even before the hormone itself was
discovered. His work provided a foundation for the modern use of
hormone therapy, such as tamoxifen, for the treatment and prevention of
breast cancer.
A half century after Beatson’s discovery, a
urologist at the University of Chicago, Charles Huggins, reported
dramatic regression of metastatic prostate cancer following removal of
the testes. Later, drugs that blocked male hormone were found to be
effective treatment for prostate cancer, and these drugs are now being
studied to determine if they have a role in prevention of prostate
cancer.
New classes of drugs (such as aromatase inhibitors, LHRH
analogs and inhibitors, and others) have substantially changed
treatment of prostate and breast cancer. Ongoing research to better
understand how hormones influence growth of some forms of cancer has
guided progress in developing and prescribing new drugs for cancer
treatment as well as for reducing the risk of developing breast and
prostate cancer.
Cancer treatments: radiation
As the 19th century was drawing to a close, in 1896 a German
physics professor, Wilhelm Conrad Roentgen, presented a remarkable
lecture entitled "Concerning a New Kind of Ray." Roentgen called it the
"X-ray", with "X" being the algebraic symbol for an unknown quantity.
There was immediate worldwide excitement. Within months, systems were
being devised to use X-rays for diagnosis, and within 3 years radiation
was used in the treatment of cancer.
In 1901 Roentgen received the first Nobel Prize awarded in
physics. Radiation therapy began with radium and with relatively
low-voltage diagnostic machines. In France a major breakthrough took
place when it was discovered that daily doses of radiation over several
weeks would greatly improve therapeutic response. The methods and the
machines for delivery of radiation therapy have steadily improved.
Today, radiation is delivered with great precision in order to destroy
malignant tumors while minimizing damage to adjacent normal tissue.
At the beginning of the 20th century, shortly after radiation
began to be used for diagnosis and therapy, it was discovered that
radiation could cause cancer as well as cure it. Many early
radiologists used the skin of their arms to test the strength of
radiation from their radiotherapy machines, looking for a dose that
would produce a pink reaction (erythema) that looked like sunburn. They
called this the "erythema dose," and this was considered an estimate of
the proper daily fraction of radiation. In retrospect, it is no
surprise that many developed leukemia.
Advances in radiation physics and computer technology during
the last quarter of the 20th century are making it possible to aim
radiation more precisely than in the past. Conformal radiation therapy
(CRT) uses CT images and special computers to very precisely map the
location of a cancer in 3 dimensions. The patient is fitted with a
plastic mold or cast to keep the body part still. The radiation beams
are matched to the shape of the tumor and delivered to the tumor from
several directions.
Intensity-modulated radiation therapy, is like CRT but
along with aiming photon beams from several directions, the intensity
(strength) of the beams can be adjusted. This gives even more control
over decreasing the radiation reaching normal tissue while delivering a
higher dose to the cancer.
A related technique, conformal
proton beam radiation therapy, uses a similar approach to
focusing radiation on the cancer. But instead of using X-rays, this
technique uses proton beams. Protons are parts of atoms that cause
little damage to tissues they pass through but are very effective in
killing cells at the end of their path. This means that proton beam
radiation can deliver more radiation to the cancer while reducing side
effects of nearby normal tissues.
Stereotactic
surgery and stereotactic
radiation therapy are terms that describe several
techniques used to deliver a large, precise radiation dose to a small
tumor. The term surgery
may be confusing because no incision is actually made. The most common
site being treated with this technique is the brain. The linear
accelerator, or a special machine known as a Gamma Knife, can be used
to deliver this treatment. Research is ongoing to produce delivery
systems to treat sites other than the brain.
Intraoperative
radiation therapy (IORT) is a form of treatment that
delivers radiation at the time of surgery directly to the cancer or the
adjacent tissues after the cancer has been removed. It is more commonly
used in abdominal or pelvic cancers and in cancers that have a tendency
to return. IORT minimizes the amount of tissue that is exposed to
radiation because normal tissues can be moved out of the way during
surgery and shielded, thus allowing a higher dose of radiation to the
cancer.
Chemical
modifiers or radiosensitizers
are substances that make cancer more sensitive to radiation. The goal
of research into these types of substances is to develop agents that
will make the tumor more sensitive without affecting normal tissues.
Research is also ongoing to find substances that may protect normal
cells from radiation.
Cancer treatments: Chemotherapy
The century of the surgeon had begun with the discovery of
anesthesia in 1846. Fifty years later, in 1896, Roentgen presented his
famous paper on the X-ray. During World War II, naval personnel who
were exposed to mustard gas as a result of a military action were found
to have toxic effects on the bone marrow cells that develop into blood
cells. During that same period, the U.S Army was studying a number of
agents related to mustard gas in order to develop more effective agents
and to develop protective measures. In the course of that work, a
compound called nitrogen
mustard was studied and found to have substantial activity
against a cancer of the lymph nodes called lymphoma. This agent served
as the model for a long series of similar but more effective agents
(called "alkylating" agents) that killed rapidly proliferating cancer
cells by damaging their DNA.
Not long after the discovery of nitrogen mustard, Sidney
Farber of Boston demonstrated that aminopterin, a compound related to
the vitamin, folic acid, produced remission in acute leukemia in
children. Aminopterin blocked a critical chemical reaction needed for
DNA replication. That drug was the predecessor of methotrexate, a
commonly used cancer treatment drug today. Since then, other
researchers discovered drugs that blocked different functions involved
in cell growth and replication. The era of chemotherapy had begun. The
first cure of metastatic cancer was obtained in 1956 when methotrexate
was used to treat a rare tumor called choriocarcinoma.
Over the years, the development and use of chemotherapy drugs
have resulted in the successful treatment of many people with cancer.
Long term remissions and even cures of many patients with Hodgkin
disease and childhood acute lymphoblastic leukemia with chemotherapy
were first reported during the 1960s, with testicular cancer following
during the next decade. Many other cancers can be controlled for long
periods of time, even if not cured, although even the most
chemosenstive forms of cancer are not always curable. Now several
approaches are being studied to improve the activity and reduce the
undesirable side effects of chemotherapy. These include:
- new drugs, new combinations of drugs, and new delivery
techniques
- novel approaches to targeting drugs more specifically at
the cancer cells (such as liposomal therapy and monoclonal antibody
therapy) to produce fewer side effects
- drugs to reduce side effects, like colony-stimulating
factors, chemoprotective agents (such as dexrazoxane and amifostine),
and antiemetics (to reduce nausea and vomiting)
- hematopoietic stem cell transplantation
- agents that overcome multidrug resistance
Liposomal
therapy is a new technique that uses chemotherapy drugs
that have been packaged inside liposomes (synthetic fat globules). This
liposome, or fatty coating, helps them penetrate the cancer cells more
selectively and decreases possible side effects (such as hair loss,
nausea, and vomiting). Examples of liposomal medications are Doxil (the
encapsulated form of doxorubicin) and Daunoxome (the encapsulated form
of daunorubicin).
Early in the 20th century, the only curable cancers were small
and localized enough to be completely removed by surgery. Later,
radiation was used after surgery to control small tumor growths that
were not surgically removed. Finally, chemotherapy was added to destroy
small tumor growths that had spread beyond the reach of the surgeon and
radiotherapist. The use of chemotherapy after surgery to destroy the
few remaining cancer cells in the body is called adjuvant therapy.
Adjuvant therapy was tested first in breast cancer and found to be
effective. It was later used in colon cancer, cancer of the testis, and
others.
A major discovery was the advantage of multiple
chemotherapeutic agents (known as combination chemotherapy) over single
agents. Some types of very fast-growing leukemias and lymphomas (tumors
involving the cells of the bone marrow and lymph nodes, respectively)
responded extremely well to combination chemotherapy, and clinical
trials led to gradual improvement of the drug combinations used. Many
of these tumors can be cured today by appropriate combination
chemotherapy.
The approach to patient treatment has become more scientific
with the introduction of clinical trials on a wide basis throughout the
world. These clinical trials compare new treatments to standard
treatments and contribute to a better understanding of treatment
benefits and risks. Clinical trials test theories about cancer learned
in the basic science laboratory and also test ideas derived from the
clinical observations on cancer patients. They are essential to
continued progress.
Cancer treatments: immunotherapy
Scientists’ understanding of the biology of cancer
cells has led to the development of biologic agents that mimic some of
the natural signals that the body uses to regulate growth. This cancer
treatment, called biological response modifier (BRM) therapy, biologic
therapy, biotherapy, or immunotherapy, has proven effective for several
cancers through the clinical trial process.
Some of these biologic agents, occurring naturally in the
body, can now be produced in the laboratory. Examples are interferons,
interleukins, and other cytokines. These agents are given to patients
to imitate or influence the natural immune response either by directly
altering the cancer cell growth or acting indirectly to help healthy
cells control the cancer.
One of the most exciting applications of biologic therapy has
come from identifying certain tumor targets, called antigens, and
aiming an antibody at these targets. This method was first used to
localize tumors in the body for diagnosis and more recently has been
used to attack cancer cells. Using technology first developed during
the 1970s, scientists can mass produce monoclonal antibodies that are
specifically targeted to chemical components of cancer cells.
Refinements to these methods, using recombinant DNA technology, have
improved the effectiveness and decreased the side effects of these
treatments. The first therapeutic monoclonal antibodies, rituximab
(Rituxan) and trastuzumab (Herceptin) were approved during the late
1990s for treating lymphoma and breast cancer, respectively. At least 9
monoclonal antibodies are already used for cancer treatment, and many
more are being studied.
Scientists are also studying vaccines to would boost the
body’s immune response to cancer cells.
Cancer treatments: Targeted therapies
Until the late 1990s nearly all drugs used in cancer treatment
(with the notable exception of hormonal treatments) worked by killing
cells that were in the process of replicating their DNA and dividing to
form 2 new cells. These chemotherapy drugs also killed some normal
cells but fortunately, had a greater effect on cancer cells.
On the other hand, targeted therapies work by influencing the
processes that control growth division, and spread of cancer cells, as
well as the signals that cause cancer cells to naturally die (in the
way normal cells when they are too old). These targeted therapies work
in several ways.
Growth signal inhibitors: Growth factors are hormone-like
substances that help tell cells when to grow and divide. Their role in
fetal growth and repair of injured tissue was first recognized during
the 1960s. Later on, they realized that abnormal forms or abnormally
high levels of the same factors contribute to the growth and spread of
cancer cells. Researchers have also started to understand how these
factors are recognized by cells, and how that recognition leads to
signals inside the cells resulting in the abnormal features of cancer
cells. Changes in these signal pathways have also been recognized as
causing the abnormal behavior of cancerous cells. During the 1980s,
scientists recognized that many of the growth factors and other
substances responsible for growth factor recognition and signaling are
actually products of oncogenes. Among the earliest targeted therapies
that block growth signals are trastuzumab (Herceptin),
gefitinib (Iressa), imatinib (Gleevec), and cetuximab (Erbitux).
Angiogenesis inhibitors: Angiogenesis is the creation of new
blood vessels. The term comes from 2 Greek words: angio, meaning "blood
vessel," and genesis, meaning "beginning." Normally, this is a healthy
process. New blood vessels, for instance, help the body heal wounds and
repair damaged body tissues. But in a person with cancer, this same
process creates new, very small blood vessels that provide a tumor with
its own blood supply and allow it to grow. Anti-angiogenesis is a form
of targeted therapy that uses drugs or other substances to stop tumors
from making new the blood vessels they need to continue growing. This
concept was first proposed by Judah Folkman in the early 1970s but it
wasn't until 2004 that the first angiogenesis inhibitor, bevicizumab
(Avastin) was approved for clinical use.
Apoptosis-inducing drugs: Apoptosis is a natural process
through which cells with DNA too damaged to repair -- such as cancer
cells -- can be forced to die. Many anticancer treatments (including
radiation and chemotherapy) cause cell changes that eventually lead to
apoptosis. But targeted drugs in this group are different, because they
are aimed specifically at the cell substances that control cell
survival and death.
Cancer survivorship
Only a few decades ago, the prognosis (outlook) for people
facing cancer was not nearly as favorable as it is today. During the
1970s, the 1 out of 2 people diagnosed with cancer survived at least
five years. Now, more than 2 out of 3 survive that long. Today there
are about 11 million cancer survivors in the United States.
Now that more people are surviving cancer, more attention than
ever is focused on the quality of life for cancer survivors. Behavioral
researchers have conducted studies to learn more about the problems
survivors face. Some of these problems are medical ones, such as
permanent side effects of treatment. Others are emotional or social
challenges, like problems getting healthcare insurance, discrimination
by employers, or that some people avoid cancer survivors because they
just don’t know what to say and are afraid to ask.
Cancer was once a word that people were afraid to speak in
public, and people rarely admitted to being a cancer survivor. Now,
many celebrities and national leaders have very openly discussed their
cancer experiences.
The twenty-first century and beyond
The growth in our knowledge of cancer biology has led to
remarkable progress in cancer prevention, early detection, and
treatment in recent years. Scientists have learned more about cancer in
the last two decades than has been learned in all the centuries
preceding. This does not change the fact, however, that all scientific
knowledge is based on the knowledge already acquired by the hard work
and discovery of our predecessors, and that much more remains to be
learned.
Cancer research is currently advancing on so many fronts that
it is difficult to choose the ones to highlight here.
More targeted
therapies: As more is learned about the molecular biology
of cancer, researchers will have more targets at which to aim their new
drugs. In addition to more monoclonal antibodies and small signaling
pathway inhibitors, researchers are developing new classes of molecules
such as antisense oligodeoxynucleotides and small interfering RNA
(siRNA).
Nanotechnology:
New technology for producing new materials that form extremely tiny
particles is leading to very promising methods for diagnostic imaging
to more accurately demonstrate the location of tumors, and for
delivering drugs more specifically and effectively into cancer cells.
Robotoic surgery:
This term refers to manipulation of surgical instruments remotely by
robotic arms and other devices controlled by a surgeon. Robotic systems
have been used for several types of cancer surgery; radical
prostatectomy is among the most common application in surgical
oncology. As mechanical and computer technology improve, some
researchers expect future systems will be able to remove tumors more
completely and with less surgical trauma than an unaided surgeon could.
RNA expression
profiling and proteomics: RNA expression profiling
permits scientists to determine relative amounts of hundreds or even
thousands or RNA molecules at one time. Knowing what proteins or RNA
molecules are present in cells can tell scientists a lot about how the
cell is behaving. In the case of cancer, it can help distinguish more
aggressive cancers from less aggressive ones, and can often help
predict which drugs the tumor is likely to respond to. Proteomic
methods are also being tested for cancer screening. For most types of
cancer, measuring the amount of one protein in the blood is not very
accurate at finding early cancers. But researchers are hopeful that
comparing the relative amounts of many proteins may be more useful, and
that knowing particular proteins are abnormally abundant and others are
less abundant can provide accurate information.
Additional resources
Encyclopedia
Britannica. See entries on Medicine, History of Cancer.
Lyons AS, Petrucelli RJ. Medicine:
An Illustrated History. New York: Harry N. Abrams
Publishers; 1978.
Shimkin MB. Contrary
to Nature: Cancer. For sale by the Superintendent of
Documents, U.S. Printing Office, Washington D.C. 20401. DHEW
Publication No (NIH) 76-720; 1976.
References
Contran R, Kumar V, Robbins S. Robbins Pathologic Basis of
Disease, 4th ed. Philadelphia, Pa: WB Saunders; 1989.
Diamandopoulus GT. Cancer: An historical perspective. Anticancer Res 1996;16:1595-1602.
Gallucci BB. Selected concepts of cancer as a disease: From
the Greeks to 1900. Oncol
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Harvey AM. Early contributions to the surgery of cancer:
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Kardinal C, Yarbro J. A conceptual history of cancer. Semin Oncol 1979;6:396-408.
Timeline: Milestones in cancer treatment. CureToday Web site.
Accessed at
http://www.curetoday.com/index.cfm/fuseaction/article.show/id/2/article_id/631
on February 15, 2009.
Progress against cancer. Cancer.Net Web site. Accessed at
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on February 15, 2009.
The history of cancer. Institut Jules Bordet Web site.
Accessed at
http://www.bordet.be/en/presentation/history/cancer_e/cancer1.htm on
February 15, 2009.
Last Medical Review: 03/09/2009
Last Revised: 03/09/2009
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