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对抗血液系统恶性肿瘤:长达200年的战争。

Battling the hematological malignancies: the 200 years' war.

作者信息

Lichtman Marshall A

机构信息

University of Rochester Medical Center, Rochester, New York 14620, USA.

出版信息

Oncologist. 2008 Feb;13(2):126-38. doi: 10.1634/theoncologist.2007-0228.

Abstract

The delineation of the hematological malignancies began near the end of the first third of the 19th century with the recognition of the similarity among cases with lymph node tumors and an enlarged spleen (Hodgkin's disease). Descriptions of chronic and acute leukemia and myeloma followed thereafter. In the first years of the 20th century the discovery of x-radiation permitted palliative orthovoltage radiation therapy of Hodgkin's disease. Following World War II, legitimate drug therapy for the hematological malignancies was introduced: nitrogen mustard, adrenocorticotropic hormone and cortisone acetate, and anti-folic acid derivatives, initially aminopterin. Today, about 14 classes of drugs (different mechanisms of action) and >50 individual agents are being used, with others under study. Several examples of agents targeting specific transcription factors or oncoproteins have been introduced. Despite remarkable progress, including the ability to cure acute leukemia in about 70% of children, cure several genetic variants of acute myelogenous leukemia in younger adults, cure some cases of lymphoma in children and younger adults, and induce prolonged remission in many affected persons, the majority of patients face an uncertain outcome and shortened life. Thus, we have much to do in the next several decades. The significant hurdles we must overcome include: the apparent infrequency of an exogenous cause that can be avoided, the exponential increase in incidence rates with age and the dramatic negative effect of aging on the results of treatment, the challenge of one trillion or more disseminated cancer cells among which are a smaller population of cancer stem cells, the profound genetic diversity of the hematological malignancies (apparently hundreds of unique genetic primary lesions), the redundant growth and survival pathways defining the cancer phenotype, the decreasing market for pharmaceutical companies as therapy becomes more specific (fewer target patients) and drug development costs become more expensive, and the significant negative long-term effects of current therapy on both children and adults. These challenges will be gradually overcome, if we (a) develop new models of cooperation among academia, industry, and government, (b) continue the growth of international participation in cancer research (more keen minds to the task), and (c) convince the governments of the world, including that of the U.S., that an investment in minimizing the effects of cancer is as important as defending against other threats to the welfare and longevity of their citizens.

摘要

血液系统恶性肿瘤的分类始于19世纪前三分之一时期接近尾声的时候,当时人们认识到淋巴结肿瘤和脾脏肿大(霍奇金病)病例之间存在相似性。此后,对慢性和急性白血病以及骨髓瘤也有了描述。20世纪初,X射线的发现使得霍奇金病能够采用姑息性的深部X线放射治疗。第二次世界大战之后,引入了针对血液系统恶性肿瘤的合理药物治疗:氮芥、促肾上腺皮质激素和醋酸可的松,以及抗叶酸衍生物,最初是氨蝶呤。如今,正在使用大约14类药物(作用机制不同)和50多种药物个体,还有其他药物正在研究中。已经引入了一些针对特定转录因子或癌蛋白的药物实例。尽管取得了显著进展,包括能够治愈约70%的儿童急性白血病、治愈年轻成人急性髓系白血病的几种基因变异型、治愈儿童和年轻成人的一些淋巴瘤病例,并使许多患者获得长期缓解,但大多数患者面临着不确定的预后和缩短的寿命。因此,在接下来的几十年里我们还有很多工作要做。我们必须克服的重大障碍包括:可避免的外源性病因明显罕见、发病率随年龄呈指数增长以及衰老对治疗结果产生巨大负面影响、一万亿或更多的播散癌细胞(其中有较少数量的癌症干细胞)带来的挑战、血液系统恶性肿瘤的深刻遗传多样性(显然有数百种独特的遗传原发性病变)、定义癌症表型的冗余生长和存活途径、随着治疗变得更加特异(目标患者减少)以及药物开发成本变得更高,制药公司的市场不断缩小,以及当前治疗对儿童和成人都有显著的长期负面影响。如果我们(a)建立学术界、产业界和政府之间新的合作模式,(b)继续扩大国际参与癌症研究的规模(让更多敏锐的头脑投身此项任务),以及(c)说服包括美国政府在内的世界各国政府,对将癌症影响降至最低的投资与抵御对其公民福利和寿命的其他威胁同样重要,那么这些挑战将逐步得到克服。

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