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Showing papers by "Bernard Fisher published in 2008"


Journal ArticleDOI
TL;DR: Clinical trials supported the thesis that operable cancer is a systemic disease and that variations in local-regional therapy are unlikely to substantially affect survival, and showed that less radical surgery is justified.
Abstract: During the 19th, and for most of the 20th century, malignant tumors were removed by mutilating radical anatomic dissection. Advances such as anesthesia, asepsis, and blood transfusion made possible increasingly more radical operations. There was no scientific rationale for the operations being performed. Surgery in the 20th century was dominated by the principles of William S. Halsted, who contended that the bloodstream was of little significance as a route of tumor cell dissemination; a tumor was autonomous of its host; and cancer was a local-regional disease that spread in an orderly fashion based on mechanical considerations. Halsted believed that both the extent and nuances of an operation influenced patient outcome and that inadequate surgical skill was responsible for the failure to cure. A new surgical era arose in 1957, when cancer surgery began to be influenced by laboratory and clinical research, with results contrary to Halstedian principles. A new hypothesis resulted in a scientific basis for cancer surgery. Clinical trials supported the thesis that operable cancer is a systemic disease and that variations in local-regional therapy are unlikely to substantially affect survival. Complex host-tumor relationships were shown to affect every aspect of cancer and, contrary to Halsted9s thesis, the bloodstream is of considerable importance in tumor dissemination. Clinical trials also have shown that less radical surgery is justified. Studies have shown that improved survival can be achieved with systemic therapy after surgery. Such therapy can reduce both the incidence of distant disease and the tumor recurrence at the tumor site after minimal surgery. The use of systemic therapy in patients who have no identifiable metastatic disease is a drastic departure from previous strategies. New technological innovations resulting from engineering research have improved the quality of life of patients by eliminating the need for some surgical procedures. Because cancer is apt to be a systemic disease, however, clinical trials are necessary to determine the effect of these modalities on patient outcome. Although technological developments will continue to play a role in cancer therapy, research in molecular biology and genetics will dictate the future status of cancer treatment and, ultimately, the future of surgery. [Cancer Res 2008;68(24):10007–20]

75 citations


Journal ArticleDOI
TL;DR: This Commentary will put into perspective two of the articles that appeared in the Journal of Clinical Oncology in 1983 that contributed to the evolution of knowledge related to breast cancer heterogeneity and consider those articles within a broader context that includes some of the other contributions to that aspect of breast cancer biology.
Abstract: This Commentary will put into perspective two of our articles that appeared in the Journal of Clinical Oncology in 1983 that contributed to the evolution of knowledge related to breast cancer heterogeneity We will consider those articles within a broader context that includes some of our other contributions to that aspect of breast cancer biology Until about 1960, physicians paid little attention to the proposition that breast cancers might be heterogeneous Although pathologic examination clearly indicated tumor heterogeneity, they considered the varied outcomes of patients following surgery to be the principal indicators of that phenomenon Anecdotal information, however, began to indicate that older patients fared better than younger patients, large tumors led to a poorer prognosis than did small tumors, and women with positive axillary nodes did worse than those with negative nodes During the late 1960s, we began to conduct clinical investigations that were aimed at defining predictors of outcome more precisely Those studies eventually led to a greater awareness of the significance of tumor heterogeneity In 1970, we were the first to report findings that we obtained from more than 2,000 breast cancer patients in several randomized trials that demonstrated that a greater incidence of treatment failure was associated with tumors that presented with increasing numbers of positive axillary nodes Our data demonstrated the propriety of grouping women according to how many of their axillary lymph nodes were tumor positive, that is, one to three or four or more That categorization subsequently became universally accepted and continues to be an important prognostic factor Other pathobiologic factors have been found to be more effective in determining therapy During the late 1960s, tumor size also began to be viewed as a marker of breast cancer heterogeneity Neoplastic surgery was based on the concept that the time of a tumor’s existence, as measured by size, determined surgical success and that the earlier the operation (ie, the smaller the tumor), the better the chance for a cure In an effort to determine the validity of that concept, we obtained information that led us to conclude that size did not necessarily relate to either “earliness” or “lateness” of a tumor and that outcome was related to tumor and/or host factors Our findings eventually led us to formulate a hypothesis that was alternative to the one on which Halstedian radical cancer surgery was based The results of clinical trials conducted to evaluate that hypothesis ultimately led to the acceptance of breast-conserving surgery in the mid-1980s Another issue that was debated during the late 1960s related to the general belief that tumor location influenced prognosis At that time, the presence of an inner quadrant or subareolar lesion evoked pessimism because it had been demonstrated that such tumors metastasized to internal mammary lymph nodes As a consequence, not only was the prognosis apt to be worse, but more extensive radical surgery was also required Information that we reported in 1969 from more than 1,000 patients failed to demonstrate that primary tumor location influenced prognosis On the contrary, our findings showed that it was the biologic nature of a breast cancer, rather than its location, that was more important for making such a determination Thus, there was no justification for anticipating that a surgical approach based on tumor location would be more rewarding than would any other approach Those findings played a significant role in the elimination of radical internal mammary lymph-node dissection for the treatment of breast cancer While our investigations were in progress, others were establishing the foundation from which the modern era of steroid hormone action would arise With the discovery of estrogen receptors (ER) and their identification in mammary tumor cells, the determination of the presence of ER in breast cancers began to achieve clinical importance It was anticipated that two categories of tumors would be identified: those with ER (which could subsequently benefit from endocrine therapy) and those without ER (which would not) It was also believed that ER status could serve as a prognostic indicator and that women whose tumors contained ER would fare better than those whose tumors did not Those findings, and the 1962 discovery of the drug tamoxifen, whose antiestrogenic properties had already been proven in animal investigations, were to have a profound effect on future research related to both the therapy and the prevention of breast cancer Although several studies were conducted with tamoxifen in a few patients with metastatic disease during the 1970s, ER determination had not been carried out in any of those trials With the increased use of tamoxifen for the management of advanced breast cancer, the need for more information about tumor ER JOURNAL OF CLINICAL ONCOLOGY C E L E B R A T I N G 2 5 Y E A R S O F J C O VOLUME 26 NUMBER 13 MAY 1 2008

33 citations