EPOCH (chemotherapy)

EPOCH is an intensive chemotherapy regimen intended for treatment of aggressive non-Hodgkin's lymphoma.[1][2]

It is often combined with rituximab. In this case it is called R-EPOCH or EPOCH-R.

[R]-EPOCH regimen consists of:

  1. (R)ituximab: an anti-CD20 monoclonal antibody, which has the ability to kill B cells, be they normal or malignant;
  2. (E)toposide: a topoisomerase inhibitor from the group of epipodofyllotoxins;
  3. (P)rednisolone: a glucocorticoid hormone that can cause apoptosis and lysis of both normal and malignant lymphocytes;
  4. (O)ncovin, also known as vincristine: a vinca alkaloid that binds to the protein tubulin, thereby preventing the formation of microtubules and mitosis;
  5. (C)yclophosphamide: an alkylating antineoplastic agent;
  6. (H)ydroxydaunorubicin, also known as doxorubicin: an anthracycline antibiotic that is able to intercalate DNA, damaging it and preventing the cell division.

Dosing regimen

DrugDoseModeDays
(R)ituximab375 mg/m2IV infusionDay 1
(E)toposide50 mg/m2IV continuous infusion over 24 hDays 1–4
(P)rednisolone60 mg/m2By mouth, twice a day (PO BID)Days 1–5
(O)ncovin: vincristine0.4 mg/m2IV continuous infusion over 24 hDays 1–4
(C)yclophosphamide750 mg/m2IV bolus given over 15 minDay 5
(H)ydroxydaunorubicin: doxorubicin10 mg/m2IV continuous infusion over 24 hDays 1–4

This regimen requires the use of prophylactic antibiotics to prevent infectious complications, as well as the use of colony-stimulating factors (G-CSF) from the first day after the end of chemotherapy to the day of full blood count restoration (ANC > 1000/μL).

There is also an improved version of the regimen. In this version the chemotherapy dose varies from cycle to cycle depending on the patient's ability to tolerate chemotherapy and the degree of neutropenia and thrombocytopenia observed in this patient after each cycle. This approach is called dose-adjusted EPOCH, or DA-EPOCH (DA-EPOCH-R, DA-R-EPOCH, R-DA-EPOCH).

Dose change rules are as follows:

Twice a week a full blood count with white blood cell count (WBC) differential is obtained.

Dose escalation above the starting doses in case of good patient's chemotherapy tolerability applies simultaneously to etoposide, doxorubicin and cyclophosphamide.

Dose de-escalation below the starting doses in case of poor patient's chemotherapy tolerability applies to cyclophosphamide only.

If the nadir ANC > 500/μL, then the doses of etoposide, doxorubicin, and cyclophosphamide for the next cycle are all increased by 20% over the doses used in the previous cycle.

If the nadir ANC < 500/μL on one or two blood checks, but ANC rises above 500 at the time of third check (i.e. the duration of agranulocytosis is less than nine days), and the nadir of platelet count is > 25,000/μL, then the dose for the next course will remain the same.

If the nadir ANC < 500/μL for 10 days or more, or if the nadir platelet count at every time falls below 25,000/μL, then the doses of etoposide, doxorubicin and cyclophosphamide are reduced by 20% below the doses used in the previous cycle, but doxorubicin and etoposide should not be reduced below the initial dose (dose in first course).[3]

gollark: In relative or absolute terms?
gollark: If you're offloading all your complex real-time computing somewhere else, then currently that means you'll probably just burn away the power savings on running your device's 4G radios and have it randomly break when bandwidth drops low enough.
gollark: The nice thing about advancing technology is that it gets more feasible as time goes on.
gollark: There *are* dedicated "AI accelerators" on modern SoCs, too, maybe that could help.
gollark: And mobile processors tend to improve in efficiency as time goes on, and then the gains get used to just make the phones thinner and run more useless background services or something.

References

This article is issued from Wikipedia. The text is licensed under Creative Commons - Attribution - Sharealike. Additional terms may apply for the media files.