A brain tumor (or brain tumour) is an
intracranial solid neoplasm, a tumor (defined as an abnormal growth of
cells) within the brain or the central spinal canal.
Brain tumors include all tumors
inside the cranium or in the central spinal canal. They are created by
an abnormal and uncontrolled cell division, normally either in the brain
itself (neurons, glial cells (astrocytes, oligodendrocytes, ependymal
cells, myelin-producing Schwann cells), lymphatic tissue, blood
vessels), in the cranial nerves, in the brain envelopes (meninges),
skull, pituitary and pineal gland, or spread from cancers primarily
located in other organs (metastatic tumors).
Any brain tumor is inherently serious
and life-threatening because of its invasive and infiltrative character
in the limited space of the intracranial cavity. However, brain tumors
(even malignant ones) are not invariably fatal. Brain tumors or
intracranial neoplasms can be cancerous (malignant) or non-cancerous
(benign); however, the definitions of malignant or benign neoplasms
differs from those commonly used in other types of cancerous or
non-cancerous neoplasms in the body. Its threat level depends on the
combination of factors like the type of tumor, its location, its size
and its state of development. Because the brain is well protected by the
skull, the early detection of a brain tumor only occurs when diagnostic
tools are directed at the intracranial cavity. Usually detection occurs
in advanced stages when the presence of the tumor has caused
unexplained symptoms.
Primary (true) brain tumors are
commonly located in the posterior cranial fossa in children and in the
anterior two-thirds of the cerebral hemispheres in adults, although they
can affect any part of the brain.
The prognosis of brain cancer
varies based on the type of cancer. Medulloblastoma has a good prognosis
with chemotherapy, radiotherapy, and surgical resection while
glioblastoma multiforme has a median survival of only 12 months even
with aggressive chemoradiotherapy and surgery. Brainstem gliomas have
the poorest prognosis of any form of brain cancer, with most patients
dying within one year, even with therapy that typically consists of
radiation to the tumor along with corticosteroids. However, one type of
brainstem glioma, a focal seems open to exceptional prognosis and
long-term survival has frequently been reported.
Tumors have characteristics that
allow pathologists to determine how dangerous a tumor is/was for the
patient, how it will evolve and it will allow the medical team to
determine the management plan for the patient.
Anaplasia: or dedifferentiation;
loss of differentiation of cells and of their orientation to one
another and blood vessels, a characteristic of anaplastic tumor tissue.
Anaplastic cells have lost total control of their normal functions and
many have deteriorated cell structures. Anaplastic cells often have
abnormally high nuclear-to-cytoplasmic ratios, and many are
multinucleated. Additionally, the nuclei of anaplastic cells are usually
unnaturally shaped or oversized nuclei. Cells can become anaplastic in
two ways: neoplastic tumor cells can dedifferentiate to become
anaplasias (the dedifferentiation causes the cells to lose all of their
normal structure/function), or cancer stem cells can increase in their
capacity to multiply (i.e., uncontrollable growth due to failure of
differentiation).
Atypia: is an indication of
abnormality of a cell (which may be indicative for malignancy).
Significance of the abnormality is highly dependent on context.
Neoplasia: is the (uncontrolled)
division of cells; as such neoplasia is not problematic but its
consequences are: the uncontrolled division of cells means that the mass
of a neoplasm increases in size, and in a confined space such as the
intracranial cavity this quickly becomes problematic because the mass
invades the space of the brain pushing it aside, leading to compression
of the brain tissue and increased intracranial pressure and destruction
of brain parenchyma. Increased Intracranial pressure (ICP) may be
attributable to the direct mass effect of the tumor, increased blood
volume, or increased cerebrospinal fluid (CSF) volume may in turn have
secondary symptoms
Necrosis: is the (premature)
death of cells, caused by external factors such as infection, toxin or
trauma. Necrotic cells send the wrong chemical signals which prevents
phagocytes from disposing of the dead cells, leading to a build up of
dead tissue, cell debris and toxins at or near the site of the necrotic
cells.
Arterial and venous hypoxia, or
the deprivation of adequate oxygen supply to certain areas of the brain,
occurs when a tumor makes use of nearby blood vessels for its supply of
blood and the neoplasm enters into competition for nutrients with the
surrounding brain tissue.
More generally a neoplasm may
cause release of metabolic end products (e.g., free radicals, altered
electrolytes, neurotransmitters), and release and recruitment of
cellular mediators (e.g., cytokines) that disrupt normal parenchymal
function.
The visibility of signs and
symptoms of brain tumors mainly depends on two factors: tumor size
(volume) and tumor location. The moment that symptoms will become
apparent, either to the person or people around him (symptom onset) is
an important milestone in the course of the diagnosis and treatment of
the tumor. The symptom onset - in the timeline of the development of the
neoplasm - depends in many cases on the nature of the tumor but in many
cases is also related to the change of the neoplasm from "benign" (i.e.
slow-growing/late symptom onset) to more malignant (fast growing/early
symptom onset).
Symptoms of solid neoplasms of the brain (primary brain tumors and secondary tumors alike) can be divided in 3 main categories :
- Consequences of intracranial hypertension : The symptoms that often occur first are those that are the consequences of increased intracranial pressure: Large tumors or tumors with extensive perifocal swelling (edema) inevitably lead to elevated intracranial pressure (intracranial hypertension), which translates clinically into headaches, vomiting (sometimes without nausea), altered state of consciousness (somnolence, coma), dilatation of the pupil on the side of the lesion (anisocoria), papilledema (prominent optic disc at the funduscopic eye examination). However, even small tumors obstructing the passage of cerebrospinal fluid (CSF) may cause early signs of increased intracranial pressure. Increased intracranial pressure may result in herniation (i.e. displacement) of certain parts of the brain, such as the cerebellar tonsils or the temporal uncus, resulting in lethal brainstem compression. In very young children, elevated intracranial pressure may cause an increase in the diameter of the skull and bulging of the fontanelles.
- Dysfunction : depending on the tumor location and the damage it may have caused to surrounding brain structures, either through compression or infiltration, any type of focal neurologic symptoms may occur, such as cognitive and behavioral impairment (including impaired judgment, memory loss, lack of recognition, spatial orientation disorders), personality or emotional changes, hemiparesis, hypoesthesia, aphasia, ataxia, visual field impairment, impaired sense of smell, impaired hearing, facial paralysis, double vision, dizziness, but more severe symptoms might occur too such as: paralysis on one side of the body hemiplegia or impairment to swallow . These symptoms are not specific for brain tumors — they may be caused by a large variety of neurologic conditions (e.g. stroke, traumatic brain injury). What counts, however, is the location of the lesion and the functional systems (e.g. motor, sensory, visual, etc.) it affects. A bilateral temporal visual field defect (bitemporal hemianopia—due to compression of the optic chiasm), often associated with endocrine disfunction—either hypopituitarism or hyperproduction of pituitary hormones and hyperprolactinemia is suggestive of a pituitary tumor.
- Irritation : abnormal fatigue, weariness, absences and tremors, but also epileptic seizures.
The above symptoms are true for
ALL types of neoplasm of the brain (including secondary tumors). It is
common that a person carry a primary benign neoplasm for several years
and have no visible symptoms at all. Many present some vague and
intermittent symptoms like headaches and occasional vomiting or
weariness, which can be easily mistaken for gastritis or
gastroenteritis. It might seem strange that despite having a mass in his
skull exercising pressure on the brain the patient feels no pain, but
as anyone who has suffered a concussion can attest, pain is felt on the
outside of the skull and not in the brain itself. The brain has no nerve
sensors in the meninges (outer surface) with which to feel or transmit
pain to the brain's pain center; it cannot signal pain without a sensory
input. That is why secondary symptoms like those described above should
alert doctors to the possible diagnosis of a neoplasm of the brain.
Although there is no specific or
singular clinical symptom or sign for any brain tumors, the presence of
a combination of symptoms and the lack of corresponding clinical
indications of infections or other causes can be an indicator to
redirect diagnostic investigation towards the possibility of an
intracranial neoplasm.
The diagnosis will often start
with an interrogation of the patient to get a clear view of his medical
antecedents, and his current symptoms. Clinical and laboratory
investigations will serve to exclude infections as the cause of the
symptoms. Examinations in this stage may include ophtamological,
otolaryngological (or ENT) and/or electrophysiological exams. The use of
electroencephalography (EEG) often plays a role in the diagnosis of
brain tumors.
Swelling, or obstruction of the
passage of cerebrospinal fluid (CSF) from the brain may cause (early)
signs of increased intracranial pressure which translates clinically
into headaches, vomiting, or an altered state of consciousness, and in
children changes to the diameter of the skull and bulging of the
fontanelles. More complex symptoms such as endocrine dysfunctions should
alarm doctors not to exclude brain tumors.
A bilateral temporal visual
field defect (due to compression of the optic chiasm) or dilatation of
the pupil, and the occurrence of either slowly evolving or the sudden
onset of focal neurologic symptoms, such as cognitive and behavioral
impairment (including impaired judgment, memory loss, lack of
recognition, spatial orientation disorders), personality or emotional
changes, hemiparesis, hypoesthesia, aphasia, ataxia, visual field
impairment, impaired sense of smell, impaired hearing, facial paralysis,
double vision, or more severe symptoms such as tremors, paralysis on
one side of the body hemiplegia, or (epileptic) seizures in a patient
with a negative history for epilepsy, should raise the possibility of a
brain tumor.
The goal of radiation therapy is
to selectively kill tumor cells while leaving normal brain tissue
unharmed. In standard external beam radiation therapy, multiple
treatments of standard-dose "fractions" of radiation are applied to the
brain. This process is repeated for a total of 10 to 30 treatments,
depending on the type of tumor. This additional treatment provides some
patients with improved outcomes and longer survival rates.
Radiosurgery is a treatment
method that uses computerized calculations to focus radiation at the
site of the tumor while minimizing the radiation dose to the surrounding
brain. Radiosurgery may be an adjunct to other treatments, or it may
represent the primary treatment technique for some tumors.
Radiotherapy may be used
following, or in some cases in place of, resection of the tumor. Forms
of radiotherapy used for brain cancer include external beam radiation
therapy, brachytherapy, and in more difficult cases, stereotactic
radiosurgery, such as Gamma knife, Cyberknife or Novalis Tx
radiosurgery.
Radiotherapy is the most common
treatment for secondary brain tumors. The amount of radiotherapy depends
on the size of the area of the brain affected by cancer. Conventional
external beam 'whole brain radiotherapy treatment' (WBRT) or 'whole
brain irradiation' may be suggested if there is a risk that other
secondary tumors will develop in the future. Stereotactic radiotherapy
is usually recommended in cases involving fewer than three small
secondary brain tumors.
Occurrence of Brain Tumors
The incidence of low-grade
astrocytoma has not been shown to vary significantly with nationality.
However, studies examining the incidence of malignant CNS tumors have
shown some variation with national origin. Since some of these
high-grade lesions arise from low-grade tumors, these trends are worth
mentioning. Specifically, the incidence of CNS tumors in the United
States, Israel, and the Nordic countries is relatively high, while Japan
and Asian countries have a lower incidence. These differences probably
reflect some biological differences as well as differences in pathologic
diagnosis and reporting.
Worldwide data on incidence of
cancer can be found at the WHO (world health organisation) and is
handled by the AIRC (Agency for Interanctional Research on Cancer)
located in France.
Figures for incidences of
cancers of the brain show a significant difference between more and less
developed countries (i.e. the lesser developed countries have less
incidences of tumors of the brain) this could be explained by
undiagnosed tumor-related deaths (patient in extreme poor situations
don't get diagnosed simply because they don't have access to the modern
diagnostic facilities required to diagnose a brain tumor) and by deaths
caused by other poverty related causes that preempt a patients life
before tumors develop or tumors become life threatening. Nevertheless
studies have been made that certain forms of primary brain tumors are
more prevalent among certain groups of the population
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