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Balancing clinical and supportive care at every step of the disease continuum

It seems it was  just yesterday that we did our first “mutation analysis” to help guide us in our treatment of patients with a drug that was more likely to work than not. Of course, I am referring to estrogen-receptor/progesterone receptor (ER/PR) blocking therapy, and “yesterday” actually goes all the way back to the 1970s! When tamoxifen was first given to unselected metastatic breast cancer patients, the response rate was low, but when the study population was “enriched” with breast cancer patients who were ER/ PR-positive, the response rates improved and the outcomes were more favorable. So began the era of tumor markers and enriching patient populations, and the process now referred to as mutation analysis, which is becoming more broadly applicable to other tumors as well.

 

Click on the PDF icon at the top of this introduction to read the full article.

 

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The Journal of Community and Supportive Oncology - 13(11)
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381-382
Legacy Keywords
estrogen-receptor, progesterone receptor, ER/PR, tamoxifen, HER2/neu, BRAF, EGFR, CINV, chemotherapy-induced nausea and vomiting, dexamethasone, lung cancer, length of stay, LoS, myelodysplastic syndrome, MDS, non-small-cell lung cancer, NSCLC

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It seems it was  just yesterday that we did our first “mutation analysis” to help guide us in our treatment of patients with a drug that was more likely to work than not. Of course, I am referring to estrogen-receptor/progesterone receptor (ER/PR) blocking therapy, and “yesterday” actually goes all the way back to the 1970s! When tamoxifen was first given to unselected metastatic breast cancer patients, the response rate was low, but when the study population was “enriched” with breast cancer patients who were ER/ PR-positive, the response rates improved and the outcomes were more favorable. So began the era of tumor markers and enriching patient populations, and the process now referred to as mutation analysis, which is becoming more broadly applicable to other tumors as well.

 

Click on the PDF icon at the top of this introduction to read the full article.

 

It seems it was  just yesterday that we did our first “mutation analysis” to help guide us in our treatment of patients with a drug that was more likely to work than not. Of course, I am referring to estrogen-receptor/progesterone receptor (ER/PR) blocking therapy, and “yesterday” actually goes all the way back to the 1970s! When tamoxifen was first given to unselected metastatic breast cancer patients, the response rate was low, but when the study population was “enriched” with breast cancer patients who were ER/ PR-positive, the response rates improved and the outcomes were more favorable. So began the era of tumor markers and enriching patient populations, and the process now referred to as mutation analysis, which is becoming more broadly applicable to other tumors as well.

 

Click on the PDF icon at the top of this introduction to read the full article.

 

Issue
The Journal of Community and Supportive Oncology - 13(11)
Issue
The Journal of Community and Supportive Oncology - 13(11)
Page Number
381-382
Page Number
381-382
Publications
Publications
Topics
Article Type
Display Headline
Balancing clinical and supportive care at every step of the disease continuum
Display Headline
Balancing clinical and supportive care at every step of the disease continuum
Legacy Keywords
estrogen-receptor, progesterone receptor, ER/PR, tamoxifen, HER2/neu, BRAF, EGFR, CINV, chemotherapy-induced nausea and vomiting, dexamethasone, lung cancer, length of stay, LoS, myelodysplastic syndrome, MDS, non-small-cell lung cancer, NSCLC

Legacy Keywords
estrogen-receptor, progesterone receptor, ER/PR, tamoxifen, HER2/neu, BRAF, EGFR, CINV, chemotherapy-induced nausea and vomiting, dexamethasone, lung cancer, length of stay, LoS, myelodysplastic syndrome, MDS, non-small-cell lung cancer, NSCLC

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JCSO 2015;13:381-382
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