CANCER MANAGEMENT IN MAN Biological Response Modifiers, Chemotherapy, Antibiotics, Hyperthermia, Supporting Measures Cancer Growth and Progression SERIES EDITOR: HANS E. KAISER Department of Pathology, University of Maryland, Baltimore, Md, U.S.A. Scientific Advisors: Kenneth W. Brunson / Harvey A. Gilbert / Ronald H. Goldfarb / Alfred L. Goldson / Elizier Gorelik / Anton Gregl / Ronald B. Herberman / James F. Holland / Ernst H. Krokowski t / Arthur S. Levine / Annabel G. Liebelt / Lance A. Liotta / Seoras D. Morrison / Thkao Ohnuma / Richard L. Schilsky / Harold L. Stewart / Jerome A. Urban / Elizabeth K. Weisburger / Paul V. Woolley Volume 1: Fundamental Aspects of Cancer Volume Editor: Ronald H. Goldfarb ISBN 0-89838-990-9 Volume 2: Mechanisms of Carcinogenesis Volume Editor: Elizabeth K. Weisburger ISBN 0-89838-991-7 Volume 3: Influence of Tumor Development on the Host Volume Editor: Lance A. Liotta ISBN 0-89838-992-5 Volume 4: Influence of the Host on Tumor Development Volume Editor: Ronald B. Herberman ISBN 0-89838-993-3 Volume 5: Comparative Aspects of Tumor Development Volume Editor: Hans E. Kaiser ISBN 0-89838-994-1 Volume 6: Etiology of Cancer in Man Volume Editor: Arthur S. Levine ISBN 0-89838-995-X Volume 7: Local Invasion and Spread of Cancer Volume Editor: Kenneth W. Brunson ISBN 0-89838-996-8 Volume 8: Metastasis / Dissemination Volume Editor: Elizier L. Gorelik ISBN 0-89838-997-6 Volume 9: Cancer Management in Man: Detection, Diagnosis, Surgery, Radiology, Chronobiology, Endocrine Therapy Volume Editor: Alfred L. Goldson ISBN 0-89838-998-4 Volume 10: Cancer Management in Man: Biological Response Modifiers, Chemotherapy, Antibiotics, Hyperthermia, Supporting Measures Volume Editor: Paul V. Woolley ISBN 0-89838-999-2 Complete set: ISBN 0-89838-989-5 Cancer Management in Man Biological Response Modifiers, Chemotherapy, Antibiotics, Hyperthermia, Supporting Measures Edited by PAUL V. WOOLLEY Division of Oncology Vincent T. Lombardi Cancer Research Center Georgetown University School of Medicine Washington, D.C., U.S.A. Kluwer Academic Publishers DORDRECHT / BOSTON / WNDON Library of Congress Cataloging in Publication Data Cancer management in man: biological response modifiers, chemotherapy. antibiotics. hyperthermia. supporting measures edited by Paul U. Woolley. p. cm. -- (Cancer growth and progression; 10) Includes index. ISBN -13: 978-94-010-6983-0 e-ISBN-13:978-94-009-1095-9 DOl: 10.1007/978-94-009-1095-9 1. Cancer--Treatment--Congresses. 2. Biological response modifiers--Therapeutic use--Congresses. 3. Cancer--Immunotherapy -Congresses. 4. Cancer--Chemotherapy--Congresses. 5. Cancer- -Adjuvant treatment--Congresses. I. Woolley. Paul V. II. Series: Cancer growth and progression; v. 10. [DNLM- 1. Antineoplastic Acents. 2. Neoplasms--drug therapv.] RC270.8.C362 1989 - 616.99'406--dc19 DNLM/DlC for Library of Congress 88-23018 CIP ISBN-13: 978-94-010-6983-0 Published by Kluwer Academic Publishers, p.o. Box 17,3300 AA Dordrecht, The Netherlands. Kluwer Academic Publishers incorporates the publishing programmes of Martinus Nijhoff, Dr W. Junk, D. Reidel, and MTP Press. Sold and distributed in the U.S.A. and Canada by Kluwer Academic Publishers, 101 Philip Drive, Norwell, MA 02061, U.S.A. In all other countries, sold and distributed by Kluwer Academic Publishers Group, P.O. Box 322, 3300 AH Dordrecht, The Netherlands. Cover design by Jos Vrolijk. All rights reserved © J 989 by Kluwer Academic Publishers Softcover reprint of the hardcover 1st edition J 989 No part of the material protected by this copyright notice may be reproduced or utilized in any form or by any means, electronic or mechanical, including photocopying, recording, or by any information storage and retrieval system, without written permission from the copyright owners. INTRODUCTION This volume, the last in this series on cancer growth and Moreover, the current status of plant-derived vinca alka progression, is a companion volume to Volume IX and loids and non-alkaloid natural products is summarized. further explores established and novel approaches for the Advances in hyperthermia and additional approaches for therapy of patients with malignant neoplasms. The stra the therapy of malignancies are also presented. tegies reflected in these volumes are direct extrapolations The volume continues with chapters on bone marrow from the basic science of cancer biology, growth and pro transplantation as well as hematologic and nutritional sup gression described in earlier volumes of this series. Some port for the cancer patient. Blood pressure in the cancer approaches are directed towards the eradication or modifi patient, therapy for nausea and vomiting as well as pain are cation of the properties of heterogeneous malignant tumor discussed. The last chapter is devoted to the problems of the cells at various stages of tumor progression, while other terminally ill, including evaluations of the burden relatives approaches are directed towards modification of the host and friends of the cancer patient have to bear. antitumor defense systems, e.g., enhancement of host anti It is clear that important advances in the basic science of tumor immune reactivity. cancer growth and progression (reviewed in Volumes I-IV The chapters reviewing immunotherapy and biological of this series) coupled with an understanding of cancer in response modifiers in cancer treatment indicate how man as compared to other species (Volume V), and an advances in the basic science of cancer biology and tumor understanding of the etiology of cancer in man (Volume VI), immunology (see Volumes I-IV) have been rapidly extended local invasion and spread of cancer in man (Volume VII), to clinical strategies for therapy of human neoplasms. In and patterns of metastasis/dissemination in man (Volume deed, these new approaches may yield effective modalities VIII) are all essential features for the formulation of new for cancer treatment with a high margin of safety and effi advances in cancer management for human neoplasms. The cacy with the capacity to overcome conventional drug resis recent and substantial advances in cancer management re tance and tumor heterogeneity. Additional approaches viewed in this volume, and in Volume IX, indicate the rapid towards cancer treatment, as well as advances in conven and expanding progress that will continue to emerge from tional treatment are also reviewed in this volume and in this continuum of basic sciences, preclinical studies in clude: transcatheter management, antifolates, purine metab therapy and diagnosis models in animals, and ultimate ex olites, alkylating agents, platinum compounds, nitro trapolation to the management of cancer in man. soureas, triazine and hydrazine derivatives, anthracycline antibiotics, actinomycin and other antitumor antibiotics. Series Editor Volume Editor Hans E. Kaiser Paul V. Woolley TABLE OF CONTENTS Introduction . . . . . . . . . V List of Contributors. . . . . . IX 1. Biological response modifiers R.K. OLDHAM. . . 2. Antitumor effects of interferons R.M. FRIEDMAN and R.K. OLDHAM . 9 3. Transcatheter management of neoplasms e.H. CARRASCO, S. WALLACE, e. CHARNSANGAVEJ and W. BECHTEL. 21 4. Antifolates M.G. NAIR. . . . . . . . . . 35 5. Purine antimetabolites W. SADEE and B.T. NGUYEN. 54 6. Alkylating agents D.E.V. WILMAN and P.B. FARMER. 63 7. Platinum compounds C.L. LITTERST and E. REED 85 8. Nitrosoureas G. POWIS . . . . . . . 98 9.Triazine and hydrazine derivatives G. POWIS . . . 113 10. Anthracyc1ine antibiotics N.R. BACHUR. . . . . 125 11. Actinomycin D.L. ANTON and P.A. FRIEDMAN 131 12. Other antitumor antibiotics G.R. LYNCH and M. LANE . 134 13. Plant alkaloids: the vinca alkaloids M.e. CASTLE . . . . . . . 147 14. Non-alkaloid natural products as anticancer agents D.G.I. KINGSTON 152 15. Hyperthermia M.W. DEWHIRST. . . . . . . . . . . . 159 16. Current advances in bone marrow transplantation for cancer treatment D.V. KIRKPATRICK and L. DELMONTE 165 17. Hematologic support of the patient with malignancy J.e. PHARES. . . . . . . . . . . . . . . . . . . . . . 180 18. The sphygmochron for chronobiologic blood pressure and heart rate assessment in cancer patients J. HALBERG, G. CORNELISSEN, FRANZ HALBERG, F. HALBERG and E. HALBERG. 189 19. Nutritional support of cancer patients during cancer progression T. OHNUMA. . . . . . . . . . . . . . . . . . . . . . . . . 196 20. Palliative chemotherapy: Cancer chemotherapy-induced nausea and vomiting J. LASZLO and V.S. LUCAS, Jr. . 204 21. Chronic pain management R.M. FRANK. . . . . . . . . . . . . . . . . . . . . . . . . 207 22. Care for the terminally ill: Death and dying H.E. KAISER, D.B. BROCK, D.J. FOLEY, H. MAIER-GERBER and T.A. HODGSON 216 Index of subjects . . . . . . . . . . . . . . . .. .................. 227 vii Inspiration and encouragement for this wide ranging project on cancer distribution and dissemination from a comparative biological and clinical point of view, was given by my late friend E. H. Krokowski. Those engaged on the project included 252 scientists. listed as contributors. volume editors and scientific advisors, and a dedicated staff. Special assistance was furnished by 1. P. Dickson, .J. A. Feulner, and I. Theloe. I. Bauer, D. L. Fisher. S. Fleishman. K. Joshi. A. M. Lewis, J. Taylor and K. E. Yinug have provided additional assistance. The firm support of the publisher. especially B. F. Commandeur. is deeply appreciated. The support of the University of Maryland throughout the preparation of the series is acknowledged. To the completion of this undertaking my wife. Charlotte Kaiser. has devoted her unslagging energy and invaluable support. CONTRIBUTORS David L. ANTON, PhD. Mark W. DEWHIRST, DVM, Ph.D. Beth Israel Hospital Medical Center Harvard Medical School Duke University 330 Brookline Avenue Durham, NC 27710, USA Boston, MA 02215, USA Current address: Peter B. FARMER, Ph.D. E.I. Du Pont De Nemours & Company MRC Toxicology Unit Medical Research Council Laboratories Wilmington, Delaware 19898, USA W oodmansterne Road Carshalton, Surrey SM5 4EF, UK Nicolas BACHUR, M.D. Maryland Cancer Center DAN J. FOLEY, M.S. University of Maryland Hospital Epidemiology, Demography & Biometry Program National 22 S. Greene Street Institute on Aging Baltimore, MD 21201, USA 7550 Wisconsin Avenue Bethesda, MD 20892, USA William BECHTEL, M.D. M.D. Anderson Hospital and Tumor Institute Robert M. FRANK, R.Ph. 6723 Bertner Avenue Department of Pharmacy Houston, Texas 77030, USA Mount Sinai School of Medicine at The Mount Sinai Hospital The Mount Sinai Medical Center of the City University Dwight B. BROCK, Ph.D. of New York Epidemiology, Demography & Biometry Program One Gustave L. Levy Place National Institute on Aging New York, NY 10029, USA 7550 Wisconsin Ave Bethesda, MD 20892, USA Paul A. FRIEDMAN, M.D. Beth Israel Hospital C. Humberto CARRASCO, M.D. Harvard Medical School M.D. Anderson Hospital and Tumor Institute 330 Brookline Avenue 6723 Bertner Avenue Boston, MA 02215, USA Houston, TX 77030, USA Current address: Merck Sharp & Dohme Research Laboratories Mickey C. CASTLE, Ph.D. Division of Merck & Co. Department of Pharmacology West Point, PA 19486, USA Eastern Virginia Medical School P.O. Box 1980 Robert M. FRIEDMAN, M.D. Norfolk, VA 23501, USA Department of Pathology Uniformed Services University of the Health Sciences Chulsip CHARNSANGAVEJ, M.D. 4301 Jones Bridge Road M.D. Anderson Hospital and Tumor Institute Bethesda, MD 20814, USA 6723 Bertner Avenue Houston, TX 77030, USA Erna HALBERG, B.S. Health Sciences Center Germaine CORNELISSEN, M.D. University of Minnesota Chronobiology Laboratories Minneapolis, Monnesota 55455, USA Department of Laboratory Medicine and Pathology University of Minnesota Francine HALBERG, M.D. Minneapolis, Minnesota 55455, USA Department of Radiation Oncology University of California Lilian DELMONTE, D.Sc. San Francisco, California 94115, USA Biomedical Communication Consultant 440 East 62nd Street Franz HALBERG, M.D. Apt.7E Chronobiology Laboratories New York, NY 10021, USA Department of Laboratory Medicine and formerly Memorial Sloan Kettering Cancer Center Pathology, University of Minnesota New York, New York Minneapolis, MN 55455, USA IX X Contributors Julia HALBERG, B.A., M.S., M.P.H., M.D. Binh T. NGUYEN, Ph.D. St. Paul-Ramsey Medical Center Department of Pharmacy St. Paul, Minnesota 55101, USA University of California, School of Pharmacy San Francisco, CA 94143, USA Thomas HODGSON, Ph.D. National Center for Health Statistics Takao OHNUMA, M.D., Ph.D. 3700 East West Highway Department of Neoplastic Diseases Hyattsville, MD 20782, USA The Mount Sinai Medical Center of the City University of New York Hans E. KAISER, D.Sc. One Gustave L. Levy Place Department of Pathology New York, NY 10029, USA University of Maryland, School of Medicine 10 S. Pine Street Robert K. Oldham, M.D. Baltimore, MD 21201, USA BTl Biological Therapy Institute Riverside Drive David G.I. KINGSTON, Ph.D. Franklin TN 37064, USA Department of Chemistry, College of Arts and Sciences Virginia Polytechnic Institute and State University John C. PHARES, M.D. Blacksburg, VA 24061, USA Hematology and Oncology Naval Hospital Dahlia V. KIRKPATRICK, M.D. Bethesda, MD 20814, USA Pediatric Oncology, Department of Pediatrics Tulane University Medical School Garth POWIS, D.phil. New Orleans, LO 70112, USA Division of Developmental Oncology Research Mayo Clinic M. LANE, M.D. Rochester, MN 55905, USA Baylor College of Medicine One Baylor Plaza, Houston, TX 77030, USA Eddie REED, Ph.D. National Cancer Institute John LASZLO, M.D. National Institutes of Health American Cancer Society, Inc. Bethesda, MD 20892, USA 3340 Peachtree Road, N.E. Atlanta Georgia 30026, USA Wolfgang SADEE, PhD. Department of Pharmacy Charles L. LITTERST, M.D. University of California, School of Pharmacy National Cancer Institute San Francisco, CA, 94143, USA National Institutes of Health Bethesda, MD 20891, USA Sidney WALLACE, M.D. Department of Diagnostic Radiology V. Sol Lucas, Jr., B.S. Pharm., R.Ph. The University of Texas, System Cancer Center Burroughs Wellcome Company M.D. Anderson Hospital & Tlimor Institute Research Triangle Park 6723 Bertner Ave., Houston, TX 77030, USA NC 27709, USA Derry E.V. WILMAN, Ph.D. Garrett R. LYNCH, M.D. Institute of Cancer Resea~ch Baylor College of Medicine Cancer Research Campaign Laboratory, Clifton Avenue Medical Oncology, Ben Taub General Hospital Sutton, Surrey, England, UK Houston, TX 77030, USA Paul V. WOOLLEY, M.D. Hartmut MAIER-GERBER, M.D. Division of Oncology Langensteinbacherhoehe Vincent T. Lombardi Cancer Research Center 7510 Karlsbad b. Karlsruhe, FRG Georgetown University School of Medicine 3800 Reservoir Road, N.W. Madhavan G. NAIR, Ph.D. Washington DC, 20007, USA Department of Bioiphemistry University of South Alabama Mobile, AL 36688, USA 1 BIOLOGICAL RESPONSE MODIFIERS ROBERT K. OLDHAM ABSTRACT response; (d) decrease transformation and/or increase differentia Biotherapy represents a new modality of cancer treatment. It uti tion (maturation) of tumor cells; lizes biologicals and biological response modifiers. Many of these (e) increase the ability of the host to tolerate damage by substances are of 'natural' origin eminating from mammalian cells cytotoxic modalities of cancer treatment. as physiologic mediators of immune response and as substances While several of these approaches involve the augmen active in the regulation of growth and maturation. With the advent tation of biological responses, an understanding of the bio of molecular biological techniques, hybridoma technology and logical properties of immune response molecules, growth computer applications, it is now possible to prepare these biological substances in highly purified form and in large quantities for use as and maturation factors and other biological substances will medicinals. The expertise required to apply these biotherapeutic assist in the development of specific molecular entities which approaches to the treatment of cancer often involves the use of can have direct actions on biological responses and/or on immunological and/or molecular biological capabilities. Because of tumor cells. Thus, one can visualize the development of the rather specialized expertise needed to understand and apply biological approaches with response modifying as well as these substances as anticancer approaches, those individuals with direct cytolytic, cytostatic, or maturational effects on tumor expertise in the application of chemotherapy to patients with cancer cells. are not necessarily well prepared for the translation of biotherapy It is clear that the mechanisms are now available for the to the clinic. Biotherapeutic approaches are broad and involve a development of biotherapy. To put these approaches into whole range of physiological responses inherent in cancer biology. The approaches needed to bring these biotherapeutic capabilities to clinical practice it is important to dispel a historical dogma the clinic need to be considered carefully and the use of new tech of immunotherapy. Biotherapy can have activity on clini niques and new methods of application should be encouraged so as cally apparent disease, and the testing is not restricted to not to inhibit these potentially powerful anticancer approaches. As situations where the tumor cell mass is imperceptible (38). natural mediators, many biologicals have much less inherent toxic Thus, the clinical trial designs for biotherapy can be similar ity than the drugs previously used in systemic cancer therapy. to those used previously for other modalities of C<;lncer Therefore, the systems for translating these substances from the treatment, as long as one is sensitive to the need to measure laboratory to the clinic should be restructured for the rapid trans both pharmacokinetics and the biological responses affected lation of biotherapy to the patient. by these approaches (34). Thus, testing is continuing for the interferons, lymphokines/cytokines, growth and maturation INTRODUCTION factors, monoclonal antibodies and immunoconjugates thereof, vaccines and cellular therapy. Biologicals could encompass any substance of biological origin but generally represent the products of the mam malian genome. With modern techniques of genetic engi HISTORICAL PERSPECTIVES neering the mammalian genome represents the new 'medi cine cabinet'. Biological response modifiers (BRM) are Given the variability of cancer's clinical presentation, it is agents and approaches whose mechanisms of action involve not surprising that randomized trials of nonspecific and the individual's own biological responses. Biologicals and specific immunotherapy, as translated from animal models, BRM can act in several ways in the biotherapy of cancer: have not been uniformly successful in cancer treatment (21, (a) augment the host's defenses by administering cells, 22). Naturally occurring cancers arise in a particular organ natural biologicals or the synthetic derivatives thereof as from one cell or a few cells under some carcinogenic stim effectors or mediators (direct or indirect) of an antitumor urits. In humans, these initial foci of cancer cells may grow response; over very long periods of time (from 1 % to 10 % of the (b) increase the individual's antitumor responses through human life span) before there is any clinical evidence of the augmentation and/or restoration or effector mechanisms disease. Dissemination of cells from initial focus may occur and/or decrease a component of the host's reaction that may at any time during the development of the primary tumor. be deleterious; Thus, growth and metastasis occur over months to years, (c) augment the individual's responses using modified allowing complex biological interactions to take place. tumor cells or vaccines to stimulate a greater response by the By contrast, experimentally induced cancer is an artificial individual or increase tumor cell sensitivity to an existing situation. The tumor cells injected into young, normal ani- P.V. Woolley (ed.), Cancer management in Man: Biological Response Modifiers, Chemotherapy, Antibiotics, Hyperthermia, Supporting Measures © 1989. Kluwer Academic Publishers, Dordrecht. ISBN-13: 978-94-010-6983-0
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