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Title: | Results with combination chemotherapy for high-risk gestational trophoblastic tumours 1989 to 2006 : retrospective non - randomized study |
Authors: | Rathnayake, R.W.M.W.K |
Issue Date: | 2010 |
Citation: | MD ( Clinical Oncology) |
Abstract: | GTT were treated with the EMA/CO regimen ( etoposide methotrexate, actinomycin D,
cyclophosphamiode, vincristine), actinomycin D, cyclophosphamide, vincristine). 42
patients had received no prior chemotherapy and 18 had received prior chemotherapy. 8 out
of 10 patients with drug resistance to EMA/CO were treated with cisplatin alone. Remaining
two were treated with EMA.EP ( addition of cisplatin). 42 patients who had received no
prior chemotherapy, 38 ( 90 percent) were in remission, 18 patients had received prior
chemotherapy and 15 ( 83 percent) were in remission; an overall survival of 88 percent for
the 60 patients. One of 61 patients dies before starting chemotherapy from extensive
disease. One of the 42 patients without prior chemotherapy died from febrile neutropenia.
The addition of cisplatin (EMA/EP) salvaged 2 of 2 ( 100 percent) who developpppped
drug resistance and one did require salvage surgery. Relapse after EMA/CO chemotherapy
is relatively uncommon ( 8 percent ) but survival is still very good with further
chemotherapy and or surgery with 10 ( 100 percent) of 10 patients obtaining a further
sustained remission. At present EMA/CO chemotherapy is the treatment of choice for
patients with high risk GTT. Its toxicity is predictable and reversible. In patients developing
resistance to EMA/CO can be successfully salvaged with high dose cisplatin or addition of
cisplatin ( EMA/EP). The high dose cisplatin is a very good option for relapse patients.
Further studies maybe needed to assess the high dose cisplatin schedule. |
URI: | http://archive.cmb.ac.lk:8080/xmlui/handle/70130/1252 |
Appears in Collections: | Masters Theses - Postgraduate Institute of Medicine |
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