User:Kenmcl2/MCL

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Mantle Cell Lymphoma
Classification and external resources
ICD-O: 9673/3
eMedicine med/1361 
MeSH C04.557.386.480.300.725.500

Mantle Cell Lymphoma (MCL) is one of the rarer of the non-Hodgkin's lymphomas, comprising about 6% of NHL cases[1]. There are only about 15,000 patients presently in the U.S. (The incidence seems to be somewhat higher in Europe.) It is difficult to treat and very seldom considered cured. Yet investigations into better treatments are very actively pursued world-wide. Median survival times were about 3 years, but are now estimated as approaching 6 years for new patients.

A list of support groups for Patients and Family Members appears below.

MCL is a subtype of B-cell lymphoma, due to CD5 positive antigen-naive pregerminal center B-cell within the mantle zone that surrounds normal germinal center follicles. MCL cells generally overexpress cyclin D1 due to a t(11:14) chromosomal translocation in the DNA. The cause is unknown and not genetic. MCL is not communicable. It essentially is an abnormal break and subsequent translocation in a gene that causes the cells to divide too early before becoming capable of helping to fight diseases. The cells also do not die as they should and therefore accumulate to expand the lymphoid system, including lymph nodes and the spleen, with non-useful cells which eventually render the system useless. They proliferate in a nodular or diffuse pattern with two main cytologic variants: typical or blastic. Typical cases are small to intermediate sized cells with irregular nuclei. Blastic (aka blastoid) variants have intermediate to large sized cells with finely dispersed chromatin and are more aggressive in nature.

Lymph Nodes of the head and neck, from Gray's Anatomy (click image to enlarge)
Lymph Nodes of the head and neck, from Gray's Anatomy (click image to enlarge)

Contents

[edit] Symptoms

Typical patients are men (the ratio of males to females is about 4:1) in their 60s and usually with advanced disease. About half have either fever, heavy night sweats, unexplained weight loss (over 10%) or some combination. Swelling of lymph nodes and spleen are usually present. Bone marrow, liver and GI tract involvement occurs in a very high percentage.

It is very common for a person to have initially noticed "a bump" on the neck or in the armpits or groin.

[edit] Diagnosis

Diagnosis generally requires stained slides of a surgically removed part of a lymph node. Other methods are also commonly used, including Cytogenetics and Fluorescence in situ hybridization (FISH). Polymerase chain reaction (PCR) and CER3 clonotypic primers are additional methods, but are less often used.

The immunophenotype profile consists of CD5+ (in about 80%)[2], CD10-/+, CD20+, CD23+/-, CD23-/+ (though plus in rare cases). Generally cyclin D1 is expressed but it may not be required. The workup for Mantle cell lymphoma is similar to the workup for many indolent lymphomas and certain aggressive lymphomas.

Mantle cell lymphoma is a systemic disease with frequent involvement of the bone marrow and gastrointestinal tract (generally showing polyposis in the lining). There is also a not-uncommon leukemic phase, marked by presence in the blood. For this reason, both the peripheral blood and bone marrow are evaluated for the presence of malignant cells. Chest, abdominal, and pelvic CT scans are routinely performed.

Since Mantle cell lymphoma may present a lymphomatous polyposis coli and colon involvement is common, colonoscopy is now considered a routine part of the evaluation. Upper endoscopy and neck CT scan may be helpful in selected cases. In some patients with the blastic variant, lumbar puncture is done to evaluate the spinal fluid for involvement.

[edit] Causes

Attempts to determine causes of MCL have failed. It is not known what causes the translocation damage to the gene. Exposure to toxins is often mentioned as a possibility. The translocation damage to a gene is required in only one cell for the cancer to begin.

[edit] Prognosis

Prognosis of MCL is problematic and indexes do not work as well due to patients presenting with advanced stage disease. Staging is used but is not very informative, since the malignant B-cells can travel freely though the lymphatic system and therefore most patients are at stage II or IV at diagnosis. Prognosis is not strongly affected by staging in MCL and the concept of metastasis does not really apply.

(The letter A after the Roman numeral indicates that normal external symptoms are not present. The Letter B indicates the symptoms are present and hence they are called “B Symptoms”.)

MCL is one of the few NHLs that can cross the boundary into the brain, yet it can be treated in that event.

There are a number of prognostic indicators that have been studied. There is not universal agreement on their importance or usefulness in prognosis.

Ki-67 is an indicator of how fast cells mature and is expressed in a range from about 10% to 90%. The lower the percentage, the lower the speed of maturity, and the more indolent the disease. Katzenberger et al Blood 2006;107:3407 graphs survival versus time for subsets of patients with varying Ki-67 indices. He shows median survival times of about one year for 61-90% Ki-67 and nearly 4 years for 5-20% Ki-67 index.

MCL cell types can aid in prognosis in a subjective way. Blastic is a larger cell type. Diffuse is spread through the node. Nodular are small groups of collected cells spread through the node. Diffuse and nodular are similar in behavior. Blastic is faster growing and it is harder to get long remissions. Some thought is that given a long time, some non-blastic MCL transforms to blastic. Although survival of most blastic patients is shorter, some data shows that 25% of blastic MCL patients survive to 5 years. That is longer than diffuse type and almost as long as nodular (almost 7 yrs).

Beta-2 microglobulin is another risk factor in MCL used primarily for transplant patients. Values less than 3 have yielded 95% overall survival to 6 yrs for auto SCT where over 3 yields a median of 44 mos overall survival for auto SCT (Khouri 03). This is not yet fully validated.

Testing for high levels of LDH in NHL patients is useful because LDH is released when body tissues break down for any reason. While it cannot be used as a sole means of diagnosing NHL, it is a surrogate for tracking tumor burden in those diagnosed by other means. The normal range is approximately 100-190.


Key Diagnostics for MCL

CT Scan - Computerized tomography scan yields 3-D images of part or whole body. Gives a large number of slices on X-ray image.

PET Scan - Generally of the whole body and shows image of where radioactive glucose is being burned at a rapid rate. That indicates with a black area that there is cancer present. Sometimes it gives a false positive.

PET scans are much more effective when fused with CT scan to show exactly where the cancer activity is located. By itself the PET is not precise in location.


[edit] Treatments

There are no proven standards of treatment for MCL and not even consensus on how to treat it. Many regimens are available and often get good response rates but patients almost always get disease progression after chemotherapy in several years. Each relapse is more difficult to treat and is generally faster. Fortunately, regimens are available that will treat relapse and progress is being made. Because of the aforementioned factors many MCL patients enroll in clinical trials to get the latest in treatments. There are four classes of treatments currently in general use: chemotherapy; immune based therapy; radioimmunotherapy and new biologic agents. And the phases of treatment are generally: Frontline following diagnosis; consolidation after frontline response to try to give longer remission; and relapse. Relapse is usually experienced multiple times.

[edit] Chemotherapy

Chemotherapy is widely used as frontline treatment and often is not repeated in relapse due to side effects. Alternate chemotherapy is sometimes used at first relapse. For frontline treatment, CHOP with Rituxan is the most common chemotherapy and often given as outpatient by IV. A stronger chemotherapy with greater side effects (mostly hematologic) is HyperCVAD often given as in-patient, with Rituxan and to generally fit patients (some of which are over 65). HyperCVAD is getting very popular and showing promising results especially with Rituxan. It can be used on some elderly over 65 but benefit seems to be only if the baseline Beta-2-MG blood test was normal. It is showing better CR and PFS than CHOP regimens. Another chemotherapy class is fludarabine monotherapy or combined with cyclophosphamide and mitoxatrone sometimes with rituximab. Cladribine and clofarabine are newer and investigated in a similar usage. Cytotoxic chemotherapies, including bendamustin, are being studied alone and with similar combinations. A long used approach is to increase chemotherapy dosage so strong that even the bone marrow is damaged and then to rescue the patient with an injection of his own pre-drawn stem cells. This gives the highest dosage therapy possible and is called Auto Stem Cell transplantation.

[edit] Immunotherapy

Immune based therapy is dominated now by the oft used and effective rituximab monoclonal antibody, sold under the trade name Rituxan (or as Mabthera in Europe). Some say it is a landmark medicine. It can have good activity against MCL alone but especially in combination with chemotherapies to prolong response duration. Rituximab essentially tags the cancer cells for destruction by the body. There are newer variations on monoclonal antibodies combined with radioactive molecules known as Radioimmunotherapy (RIT). These include Zevalin and Bexxar.

[edit] Targeted Therapy

New targeted agents include the proteosome inhibitor Velcade and mTor inhibitors such as temsirolimus.

[edit] External Links

[edit] Discussion Groups for Patients and Family Members

[edit] Further Reading


[edit] References

  1. ^ Mantle Cell Lymphoma[1]
  2. ^ Stanford School of Medicine: "Mantle Cell Lymphoma, Differential Diagnosis" [2]

[edit] MultiMedia