M. de Wet scite author profile

M. de Wet

4Publications

11Citation Statements Received

68Citation Statements Given

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Steve Biko Hospital, University of Pretoria

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Small Cell Lung Cancer: Analysis of Factors Influencing the Response to Treatment and Survival

Wet¹,

Falkson²,

Rapoport³

1994

Oncology

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The aims of this study were to identify prognostic factors in patients (pts) with small cell lung cancer and to identify dominant prognostic factors independent of disease stage, to define prognostic subsets through recursive partitioning and amalgamation (RPA) and to analyze the clinical characteristics of long-term survivors. The prognostic significance of 27 pre-treatment variables was evaluated in 144 pts seen at a single institution. The current study confirmed the superior outcome for pts with limited disease (LD) in terms of response, response duration, time to treatment failure and survival when compared to those with extensive disease (ED). None of the variables independently predicted for response in patients with LD. Response correlated significantly with a good performance status (PS) for pts with ED and for the whole group. A good PS was the most significant predictor for prolonged survival in pts with LD. In ED a longer survival was associated with a normal pre-treatment albumin value, absence of weight loss and female gender. When the whole group was considered, PS and number of metastatic sites were identified as the most influential factors for survival independent of disease stage. RPA analysis defined 3 prognostic subsets based on stage of disease, PS and number of metastatic sites. The best survival rates were seen in pts with LD with a good PS and pts with ED, only one metastatic site and a good PS. 11 % of pts survived > 2 years (18% LD, 6% ED). A complete response to chemotherapy was the most important predictor for long-term survival. Comparison of the data from this study with published results of protocol studies showed similar outcomes.

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Repeated use of granisetron in patients receiving cytostatic agents

Wet

Falkson

Rapoport

1993

Cancer

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Background. Granisetron was shown to be a safe and effective antiemetic agent when given with initial cytostatic therapy. This study was undertaken to investigate the efficacy and safety of the continued use of granisetron. Methods. Ninety‐one patients were given 438 cycles of granisetron during subsequent courses of cytostatic treatment. In 56 patients, 40 μg/kg IV was given in 159 cycles, and in 42 patients, 3 mg IV was given in 279 cycles. In patients having breakthrough symptoms, as many as two rescue doses were given to re‐establish control. Results. Overall objective control of nausea and vomiting was observed in 88.6% of the 40 μg/kg‐cycles and in 90.32% of the 3‐mg cycles. In the 438 cycles given, complete control was achieved in 105 of 159 (66%) of the 40‐μg/kg cycles and in 217 of 279 (77.78%) of the 3‐mg cycles. Thirty‐three patients received 97 cycles of cisplatin‐based regimens. The objective control rate was 82.47% (80 of 97 cycles) in these patients. The control rate in patients receiving regimens not containing cisplatin was 94.4% (322 of 341 cycles). Rescue doses improved or resolved symptoms in 53 of 61 (86.9%) cycles. No statistically significant difference in nausea and vomiting control was seen between men and women or between the different age groups. The only toxicities encountered were headache in 14 of 438 (3.2%) cycles and mild constipation in 8 of 438 (1.8%) cycles. Conclusion. Granisetron is safe and well tolerated, maintains its antiemetic efficacy after repeated cycles of therapy, and is effective as an interventional treatment for nausea and vomiting.

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Suramin in combination with mitomycin C in hormone-resistant prostate cancer. A phase II clinical study

et al. 1993

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A phase II clinical study of suramin in combination with mitomycin C in patients with non small cell lung cancer

et al. 1991

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M. de Wet

Small Cell Lung Cancer: Analysis of Factors Influencing the Response to Treatment and Survival

Repeated use of granisetron in patients receiving cytostatic agents

Suramin in combination with mitomycin C in hormone-resistant prostate cancer. A phase II clinical study

A phase II clinical study of suramin in combination with mitomycin C in patients with non small cell lung cancer

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