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{{ Mantle cell lymphoma }}
{{Mantle cell lymphoma }}


{{CMG}}; {{AE}} {{AS}}
{{CMG}}; {{AE}} {{Akram}}


==Overview==
==Overview==
The predominant therapy for mantle cell lymphoma is [[chemotherapy]]. Adjunctive immune based therapy, [[radioimmunotherapy]], and new biologic agents may be required.
 
The mainstay of treatment for mantle cell lymphoma is [[chemotherapy]]. However, [[immunotherapy]], [[radioimmunotherapy]], [[targeted therapy]] using newer biologic agents and [[stem cell transplantation]] are also used along with [[chemotherapy]] to treat the [[disease]]. Mantle cell lymphoma shows a heterogeneous [[clinical]] behavior, with some patients having [[Indolent mantle cell lymphoma|indolent]] [[disease]] whereas a vast majority show aggressive presentation. Most of the patients eventually [[relapse]] and have [[disease]] progression after treatment. Hence, mantle cell lymphoma is still considered an incurable [[disease]] and there is no consensus among [[Oncologist|oncologists]] about its optimal treatment. It is therefore recommended that mantle cell lymphoma patients are seen by physicians having extensive experience in dealing with mantle cell lymphoma and they are also encouraged to participate in [[Clinical trial|clinical trials]] to get the latest treatments.
 
==Medical Therapy==
==Medical Therapy==
There are no proven standards of treatment for mantle cell lymphoma, and not even consensus among specialists on how to treat it optimally. Many regimens are available and often get good response rates, but patients almost always get disease progression after chemotherapy. Each relapse is typically more difficult to treat, and relapse is generally faster. Fortunately, regimens are available that will treat relapse, and new approaches are under test. Because of the aforementioned factors, many MCL patients enroll in clinical trials to get the latest treatments.  
Mantle cell lymphoma shows a heterogeneous clinical behavior, with some patients having [[Indolent mantle cell lymphoma|indolent disease]] whereas a vast majority show aggressive presentation. Most of the patients eventually [[relapse]] and have [[disease]] progression after treatment. Hence, mantle cell lymphoma is still considered an incurable disease and there is no consensus among [[oncologists]] about its optimal treatment. It is therefore recommended that mantle cell lymphoma patients are seen by [[Physician|physicians]] having extensive experience in dealing with mantle cell lymphoma and they are also encouraged to participate in [[Clinical trial|clinical trials]] to get the latest treatments.  
*There are four classes of treatments currently in general use:  
*Different types of treatment currently being used to treat mantle cell lymphoma are as follows:  
:* [[Chemotherapy]]  
** [[Chemotherapy]]  
:* Immune based therapy
** [[Immunotherapy]]
:* [[Radioimmunotherapy]]  
** [[Radioimmunotherapy]]  
:* New biologic agents  
** [[Targeted therapy]] using newer biologic agents  
*The phases of treatment are generally:  
** [[Stem cell transplantation]]
:* Frontline
 
:* Following diagnosis
=== Stage I-II: ===
:* Consolidation
* [[Radiotherapy]] alone or combination chemoimmunotherapy with or without [[radiotherapy]] is recommended.<ref>https://www.nccn.org/professionals/physician_gls/pdf/b-cell.pdf</ref>
:* After frontline response (to prolong remissions)
* For patients with complete response(CR), clinical follow up is conducted every 3-6 months for 5 years, and then on a yearly basis.
:* Relapse (Relapse is usually experienced multiple times.)
* For patients treated with [[radiotherapy]] alone initially, [[disease]] progression and [[Relapse|relapses]] after a CR or partial response(PR) is treated with first-line induction therapy (recommended for stage II bulky and stage II-IV disease)
* For patients treated with chemoimmunotherapy with or without [[radiotherapy]], [[disease]] progression and [[Relapse|relapses]] after a CR or PR is treated with second-line therapy regimens (recommended for stage II bulky and stage II-IV disease)
 
=== Stage II (bulky) and Stage III-IV: ===
 
==== First-line induction therapy: ====
* Aggressive therapy:<ref>https://www.nccn.org/professionals/physician_gls/pdf/b-cell.pdf</ref>
**Hyper-[[CVAD regimen|CVAD]] ([[cyclophosphamide]], [[vincristine]], [[doxorubicin]] (also known by its trade name, [[Adriamycin]]), and [[dexamethasone]]) + [[rituximab]]
**Dose-intensified [[CHOP]] ([[cyclophosphamide]], [[Doxorubicin|hydroxydaunorubicin]], [[Vincristine|oncovin]] ([[vincristine]]) and [[prednisone]]) alternating with [[rituximab]] + high-dose [[cytarabine]] (NORDIC regimen)
**[[Rituximab]] and [[methotrexate]] with augmented [[CHOP]]
**Sequential [[R-CHOP regimen|R-CHOP]] and [[R-ICE regimen|R-ICE]] ([[Ifosfamide]], [[carboplatin]], [[etoposide]])
**Alternating [[R-CHOP regimen|R-CHOP]] and [[DHAP regimen|R-DHAP]] ([[Dexamethasone]], High dose Ara-C [[Cytarabine]], [[Cisplatin|Platinol]])
* Less aggressive therapy:
**[[Bendamustine]] + [[rituximab]]
**[[Bortezomib]], [[rituximab]], [[cyclophosphamide]], [[doxorubicin]], and [[prednisone]] (VR-CAP)
**[[Cladribine]] + [[rituximab]]
**[[CHOP regimen|CHOP]] + [[rituximab]] ([[R-CHOP regimen|R-CHOP]])
**Modified Hyper-[[CVAD regimen|CVAD]] with [[rituximab]] maintainence in patients older than 65 years.
* For patients with CR to first-line therapies, HDT/ASCR (High dose therapy/Autologous Stem Cell Rescue) or [[clinical trial]] participation is recommended. Follow up is conducted every 3-6 months for 5 years, and then on a yearly basis.
* For patients with PR to first-line therapies, second-line therapies may be considered.
 
==== First-line consolidation therapy: ====
* HDT/ASCR is recommended.<ref>https://www.nccn.org/professionals/physician_gls/pdf/b-cell.pdf</ref>
* Patients who are not HDT/ASCR candidates, and are in remission after [[R-CHOP]] therapy, may get [[rituximab]] maintenance therapy every 8 weeks.
 
==== Second-line therapy: ====
* The following therapies may be used in [[Relapse|relapsed]]/[[refractory]] disease:<ref>https://www.nccn.org/professionals/physician_gls/pdf/b-cell.pdf</ref>
**[[Bendamustine]] +/- [[rituximab]]
**[[Bortezomib]] +/- [[rituximab]]
**[[Cladribine]] +/- [[rituximab]]
**FC ([[fludarabine]], [[cyclophosphamide]]) +/- [[rituximab]]
**FCMR ([[fludarabine]], [[cyclophosphamide]], [[mitoxantrone]], [[rituximab]])
**FMR ([[fludarabine]], [[mitoxantrone]], [[rituximab]])
**[[Lenalidomide]] +/- [[rituximab]]
**PCR ([[pentostatin]], [[cyclophosphamide]], [[rituximab]])
**PEPC ([[prednisone]], [[etoposide]], [[procarbazine]], [[cyclophosphamide]]) +/- [[rituximab]]
**[[Ibrutinib]]
* [[Autologous bone marrow transplantation|Autologous stem cell transplant]] and [[Allogeneic stem cell transplantation|allogeneic stem cell transplant]] can be used as second-line maintenance therapy for patients in [[Remission (medicine)|remission]] with [[Relapse|relapsed]] or [[refractory]] disease.


===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.
====Frontline treatment====
* Drug Regimen: [[CHOP]] (IV) ([[Cyclophosphamide]], {{and}} [[Doxorubicin]], {{and}} [[Vincristine]], {{and}} [[Prednisone]]) {{plus}} [[Rituximab]] 
* Drug Regimen: [[Fludarabine]]
* Drug Regimen: [[Fludarabine]] {{withorwithout}} ([[Cyclophosphamide]] {{and}} [[Mitoxantrone]] {{and}} [[Rituximab]])
====Elderly(over 65) patients, baseline beta-2 microglobulin blood test was normal====
Hyper-CVAD chemotherapy consists of two combinations of drugs (courses A and B) given in an alternating fashion. The term 'hyper' refers to the hyperfractionated nature of the chemotherapy, which is given in smaller doses, more frequently, to minimize side effects. HyperCVAD is becoming popular and showing promising results, especially with rituximab. It is showing better complete remissions (CR) and progression free survival (PFS) than CHOP regimens
* Drug Regimen: (CVAD) Course A:[[Cyclophosphamide]], {{and}} [[Vincristine]], {{and}} [[Doxorubicin]], {{and}} [[Dexamethasone]] ; Course B : [[Methotrexate]] {{and}} [[Cytarabine]]   
====Relapsed patients====
* Drug regimen: PEP-C (oral), [[Prednisone]], {{and}} [[Etoposide]], {{and}} [[Procarbazine]], {{and}} [[Cyclophosphamide]][http://www.asco.org/ASCO/Abstracts+&+Virtual+Meeting/Abstracts?&vmview=abst_detail_view&confID=23&abstractID=104642].
* [[Chemotherapy]] {{withorwithout}} [[Total body irradiation]] (TBI)
===Immunotherapy===
[[Immunotherapy|Immune-based therapy]] is dominated now by the oft used and effective [[rituximab]] monoclonal antibody. It can have good activity against mantle cell lymphoma 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]].
===Targeted Therapy===
New targeted agents include the proteasome inhibitor [[Velcade]] and mTor (mammalian target of rapamycin) inhibitors such as [[Torisel|temsirolimus]].
==References==
==References==
{{Reflist|2}}
{{Reflist|2}}
{{Hematology}}


[[Category:Blood disorders]]
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{{WH}}
{{WS}}

Latest revision as of 22:37, 29 July 2020

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Ali Akram, M.B.B.S.[2]

Overview

The mainstay of treatment for mantle cell lymphoma is chemotherapy. However, immunotherapy, radioimmunotherapy, targeted therapy using newer biologic agents and stem cell transplantation are also used along with chemotherapy to treat the disease. Mantle cell lymphoma shows a heterogeneous clinical behavior, with some patients having indolent disease whereas a vast majority show aggressive presentation. Most of the patients eventually relapse and have disease progression after treatment. Hence, mantle cell lymphoma is still considered an incurable disease and there is no consensus among oncologists about its optimal treatment. It is therefore recommended that mantle cell lymphoma patients are seen by physicians having extensive experience in dealing with mantle cell lymphoma and they are also encouraged to participate in clinical trials to get the latest treatments.

Medical Therapy

Mantle cell lymphoma shows a heterogeneous clinical behavior, with some patients having indolent disease whereas a vast majority show aggressive presentation. Most of the patients eventually relapse and have disease progression after treatment. Hence, mantle cell lymphoma is still considered an incurable disease and there is no consensus among oncologists about its optimal treatment. It is therefore recommended that mantle cell lymphoma patients are seen by physicians having extensive experience in dealing with mantle cell lymphoma and they are also encouraged to participate in clinical trials to get the latest treatments.

Stage I-II:

  • Radiotherapy alone or combination chemoimmunotherapy with or without radiotherapy is recommended.[1]
  • For patients with complete response(CR), clinical follow up is conducted every 3-6 months for 5 years, and then on a yearly basis.
  • For patients treated with radiotherapy alone initially, disease progression and relapses after a CR or partial response(PR) is treated with first-line induction therapy (recommended for stage II bulky and stage II-IV disease)
  • For patients treated with chemoimmunotherapy with or without radiotherapy, disease progression and relapses after a CR or PR is treated with second-line therapy regimens (recommended for stage II bulky and stage II-IV disease)

Stage II (bulky) and Stage III-IV:

First-line induction therapy:

First-line consolidation therapy:

  • HDT/ASCR is recommended.[3]
  • Patients who are not HDT/ASCR candidates, and are in remission after R-CHOP therapy, may get rituximab maintenance therapy every 8 weeks.

Second-line therapy:

References