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Most types of cancers are assigned numbered stages to describe
their extent in the body, based on the size of the tumor and how far
the cancer has spread.
Acute lymphocytic leukemia (ALL), on the other hand, does not
usually form tumor masses. It generally affects all of the bone marrow
in the body and, in many cases, may have spread to other organs, such
as the liver, spleen, and lymph nodes. Therefore the outlook for the
patient with ALL depends on other information, such as the subtype of
ALL (determined by lab tests), the age of the patient, and other lab
test results.
Different systems have been used to classify ALL into
subtypes.
The French-American-British (FAB)
classification
In the 1970s, a group of French, American, and British (FAB)
leukemia experts divided ALL into 3 subtypes. The FAB system was based
only on the way the leukemia cells looked under the microscope after
routine staining.
French-American-British
(FAB) Classification of ALL
| FAB Subtype |
Approximate
% of Adult ALL Patients |
Immunologic
Type |
Comments |
| L1 |
30% |
T cell or pre-B cell |
|
| L2 |
65% |
T cell or pre-B cell |
|
| L3 |
5% |
B cell |
Poor prognosis with
standard therapy. Also called Burkitt leukemia. |
This system has largely been replaced, as newer lab tests now
allow doctors to classify ALL more accurately.
Classification based on immunophenotype
More recently, doctors have found that cytogenetic tests, flow
cytometry, and other lab tests provide more detailed information about
the subtype of ALL and the patient's prognosis. These tests help divide
ALL into groups based on the immunophenotype
of the leukemia, which takes into account the type of lymphocyte (B
cell or T cell) the leukemia cells come from and on how mature these
cells are. These groups have largely replaced the FAB classification.
The subtypes of ALL are now named as follows:
B-cell ALL
- early pre-B ALL (also called pro-B ALL) -- about 10% of
cases
- common ALL - about 50% of cases
- pre-B ALL - about 10% of cases
- mature B-cell ALL (Burkitt leukemia) -- about 4% of cases
T-cell ALL
- pre-T ALL - about 5% to 10% of cases
- mature T-cell ALL - about 15% to 20% of cases
The subtypes of ALL carry slightly different outlooks, but
other factors (like gene changes in the leukemia cells) may also have
an impact. Some of these prognostic factors are listed in the next
section.
Mixed lineage acute leukemias
In recent years, newer lab tests have shown that a small
number of ALL cases actually have both lymphocytic and myeloid
features. Sometimes the leukemia cells have both myeloid and
lymphocytic traits in the same cells. In other cases, a leukemia
patient may have some cells with myeloid features and others with
lymphocytic features. These types of leukemias may be called mixed
lineage leukemia, ALL with myeloid markers (My+ ALL), AML with lymphoid
markers, or biphenotypic acute leukemia (BAL).
Most studies suggest these leukemias tend to have a poorer
outlook than standard subtypes of ALL or AML. There is no standard
treatment for these leukemias. Intensive treatment (such as stem cell
transplant) is often used when possible, as they have a high risk of
recurrence after treatment.
Prognostic factors
As leukemia treatment has improved over the years, research
has focused on why some patients have a better chance for cure than
others. Differences among patients that affect response to treatment
are called prognostic factors. They help doctors decide if people with
a certain type of leukemia should get more or less treatment. These prognostic factors
include the patient's age, white blood cell count, ALL subtype,
cytogenetic test results, and response to chemotherapy.
Adult acute lymphocytic leukemia prognostic
factors
- Age:
Younger patients tend to have a better prognosis than older patients.
There is no set cutoff for this, but generally those younger than 50 do
better than those in their 50s, while people in their 50s do better
than those in their 60s or older.
- Initial white
blood cell count: People with a lower WBC count (less than
30,000 for B-cell ALL and less than 100,000 for T-cell ALL) at the time
of diagnosis tend to have a better prognosis.
- ALL subtype:
In general, T-cell ALL has a better prognosis, while mature B-cell ALL
(Burkitt leukemia) has a poorer prognosis. Other subtypes of B-cell ALL
fall somewhere in between. It's important to note that this doesn't
apply to all cases. For instance, some subtypes of T-cell ALL have a
better outlook than others.
- Chromosome
translocations: The presence of Philadelphia chromosome
(a translocation between chromosomes 9 and 22), which is found in 25%
to 30% of ALL cases, predicts a poorer prognosis. The same is true of a
translocation between chromosomes 4 and 11, which is found in about 5%
of cases.
- Response to
chemotherapy: Patients who achieve a complete remission
(no evidence of leukemia remaining) within 4 to 5 weeks of starting
treatment tend to have a better prognosis than those in whom this takes
longer. Patients who don't achieve a complete remission at all have a
poorer outlook. The prognostic value of minimal residual disease
(described below) is still being studied.
Status of acute lymphocytic leukemia after
treatment
How well a leukemia responds to treatment has an effect on
long-term prognosis.
A remission
(complete remission)
is usually defined as having no evidence of disease after treatment.
This means the bone marrow contains fewer than 5% blast cells, the
blood cell counts are within normal limits, and there are no signs or
symptoms of the disease. A molecular
complete remission means there is no evidence of leukemia
cells in the bone marrow, even when using very sensitive lab tests,
such as PCR.
Minimal
residual disease is a term used after treatment when
leukemia cells can't be found in the bone marrow using standard lab
tests (such as looking at cells under a microscope), but more sensitive
tests (such as flow cytometry or PCR) find evidence that leukemia cells
remain in the bone marrow.
Active disease
means that either there is evidence that the leukemia is still present
during treatment or that the disease has relapsed (come back) after
treatment. For a patient to be in relapse, they must have more than 5%
blast cells present in the bone marrow.
Last Medical Review: 07/23/2009
Last Revised: 07/23/2009
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