Kerr K M
Department of Pathology, Aberdeen Royal Infirmary and Aberdeen University Medical School, Foresterhill, Aberdeen AB25 2ZD, UK.
J Clin Pathol. 2001 Apr;54(4):257-71. doi: 10.1136/jcp.54.4.257.
Advances in molecular biology have increased our knowledge of the biology of preneoplastic lesions in the human lung. The recently published WHO lung tumour classification defines three separate lesions that are regarded as preinvasive neoplasia. These are (1) squamous dysplasia and carcinoma in situ (SD/CIS), (2) atypical adenomatous hyperplasia (AAH), and (3) diffuse idiopathic pulmonary neuroendocrine cell hyperplasia (DIP-NECH). SD/CIS is graded in four stages (mild, moderate, severe, and CIS), based upon the distribution of atypical cells and mitotic figures. Most airways showing SD/CIS demonstrate a range of grades; many epithelia are hard to assess and the reproducibility of this complex system remains to be established. Detailed criteria are, however, welcome and provide an objective framework on which to compare various molecular changes. Alterations in gene expression and chromosome structure known to be associated with malignant transformation can be demonstrated in CIS, less so in dysplasias, but also in morphologically normal epithelium. The changes might be sequential, and their frequency and number increase with atypia. Less is known of the "risk of progression" of SD/CIS to invasive "central" bronchial carcinoma. It may take between one and 10 years for invasion to occur, yet the lesion(s) may be reversible if carcinogen exposure ceases. AAH may be an important precursor lesion for peripheral "parenchymal" adenocarcinoma of the lung: the "adenoma" in an adenoma-carcinoma sequence. There is good morphological evidence that AAH may progress from low to high grade to bronchioloalveolar carcinoma (BAC; a non-invasive lesion by definition). Invasion then develops within BAC and peripheral lung adenocarcinoma evolves. The molecular events associated with this progression are not well understood and studies are hampered by a lack of clear criteria to distinguish high grade AAH from BAC. Nonetheless, as with SD/CIS, the patterns of expression of tumour associated genes are consistent with neoplastic progression. We have little idea of the incidence of AAH in the normal or "smoking" populations. It is found more frequently in cancer bearing lungs, especially in those with adenocarcinoma, and is more common in women. No data are available on the risk of progression of AAH. DIPNECH is an exceptionally rare lesion associated with the development of multiple carcinoid tumours. Almost nothing is known of its biology. Knowledge of these lesions will be crucial in the design and understanding of lung cancer screening programmes, where it is likely that the morphological and, more importantly perhaps, the molecular characteristics of these lesions will provide useful targets for detection and possibly even treatment.
分子生物学的进展增进了我们对人类肺癌癌前病变生物学特性的了解。最近发布的世界卫生组织(WHO)肺肿瘤分类定义了三种被视为浸润前肿瘤形成的不同病变。它们分别是:(1)鳞状上皮发育异常和原位癌(SD/CIS);(2)非典型腺瘤样增生(AAH);(3)弥漫性特发性肺神经内分泌细胞增生(DIP-NECH)。SD/CIS根据非典型细胞和有丝分裂象的分布分为四个阶段(轻度、中度、重度和原位癌)。大多数显示SD/CIS的气道呈现出一系列分级;许多上皮难以评估,并且这个复杂系统的可重复性仍有待确定。然而,详细的标准是受欢迎的,并且提供了一个客观框架,用于比较各种分子变化。已知与恶性转化相关的基因表达和染色体结构改变在原位癌中可以得到证实,在发育异常中较少见,但在形态学正常的上皮中也存在。这些变化可能是连续的,并且它们的频率和数量随着异型性增加。对于SD/CIS进展为浸润性“中央型”支气管癌的“进展风险”了解较少。浸润可能需要1至10年才会发生,然而,如果致癌物暴露停止,病变可能是可逆的。AAH可能是肺外周“实质”腺癌的一个重要前体病变:即腺癌-癌序列中的“腺瘤”。有充分的形态学证据表明,AAH可能从低级别进展到高级别,进而发展为细支气管肺泡癌(BAC;根据定义为非浸润性病变)。然后在BAC内发生浸润,外周肺腺癌逐渐形成。与这种进展相关的分子事件尚未完全了解,并且由于缺乏区分高级别AAH和BAC的明确标准,研究受到阻碍。尽管如此,与SD/CIS一样,肿瘤相关基因的表达模式与肿瘤进展一致。我们对正常或“吸烟”人群中AAH的发生率了解甚少。它在患癌肺组织中更常见,尤其是在腺癌患者中,并且在女性中更普遍。关于AAH进展风险没有可用数据。DIPNECH是一种极其罕见的病变,与多发性类癌肿瘤的发生相关。对其生物学特性几乎一无所知。了解这些病变对于肺癌筛查计划的设计和理解至关重要,在肺癌筛查中,这些病变的形态学特征,更重要的可能是分子特征,可能为检测甚至治疗提供有用的靶点。
