Ductal Carcinoma in Situ: Molecular Changes Accompanying Disease Progression.

IF 3 4区 医学 Q2 ENDOCRINOLOGY & METABOLISM
Gemma M Wilson, Phuong Dinh, Nirmala Pathmanathan, J Dinny Graham
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引用次数: 8

Abstract

Ductal carcinoma in situ (DCIS) is a non-obligate precursor of invasive ductal carcinoma (IDC), whereby if left untreated, approximately 12% of patients develop invasive disease. The current standard of care is surgical removal of the lesion, to prevent potential progression, and radiotherapy to reduce risk of recurrence. There is substantial overtreatment of DCIS patients, considering not all DCIS lesions progress to invasive disease. Hence, there is a critical imperative to better predict which DCIS lesions are destined for poor outcome and which are not, allowing for tailored treatment. Active surveillance is currently being trialed as an alternative management practice, but this approach relies on accurately identifying cases that are at low risk of progression to invasive disease. Two DCIS-specific genomic profiling assays that attempt to distinguish low and high-risk patients have emerged, but imperfections in risk stratification coupled with a high price tag warrant the continued search for more robust and accessible prognostic biomarkers. This search has largely turned researchers toward the tumor microenvironment. Recent evidence suggests that a spectrum of cell types within the DCIS microenvironment are genetically and phenotypically altered compared to normal tissue and play critical roles in disease progression. Uncovering the molecular mechanisms contributing to DCIS progression has provided optimism for the search for well-validated prognostic biomarkers that can accurately predict the risk for a patient developing IDC. The discovery of such markers would modernize DCIS management and allow tailored treatment plans. This review will summarize the current literature regarding DCIS diagnosis, treatment, and pathology.

Abstract Image

原位导管癌:伴随疾病进展的分子变化
原位导管癌(DCIS)是浸润性导管癌(IDC)的非专性前体,如果不治疗,约12%的患者会发展为浸润性疾病。目前的护理标准是手术切除病变,以防止潜在的进展,并进行放射治疗,以降低复发风险。考虑到并非所有DCIS病变都进展为侵袭性疾病,DCIS患者的治疗严重过度。因此,迫切需要更好地预测哪些DCIS病变注定会导致不良结果,哪些不会,以便进行量身定制的治疗。主动监测目前正在作为一种替代管理实践进行试验,但这种方法依赖于准确识别进展为侵袭性疾病的低风险病例。已经出现了两种DCIS特异性基因组图谱分析,试图区分低风险和高风险患者,但风险分层的缺陷加上高昂的价格标签,保证了继续寻找更强大和更容易获得的预后生物标志物。这项研究在很大程度上使研究人员转向了肿瘤微环境。最近的证据表明,与正常组织相比,DCIS微环境中的一系列细胞类型在遗传和表型上发生了改变,并在疾病进展中发挥着关键作用。揭示导致DCIS进展的分子机制为寻找能够准确预测患者患IDC风险的经充分验证的预后生物标志物提供了乐观的前景。这些标志物的发现将使DCIS管理现代化,并允许制定量身定制的治疗计划。这篇综述将总结目前有关DCIS诊断、治疗和病理学的文献。
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来源期刊
Journal of Mammary Gland Biology and Neoplasia
Journal of Mammary Gland Biology and Neoplasia 医学-内分泌学与代谢
CiteScore
5.30
自引率
4.00%
发文量
22
期刊介绍: Journal of Mammary Gland Biology and Neoplasia is the leading Journal in the field of mammary gland biology that provides researchers within and outside the field of mammary gland biology with an integrated source of information pertaining to the development, function, and pathology of the mammary gland and its function. Commencing in 2015, the Journal will begin receiving and publishing a combination of reviews and original, peer-reviewed research. The Journal covers all topics related to the field of mammary gland biology, including mammary development, breast cancer biology, lactation, and milk composition and quality. The environmental, endocrine, nutritional, and molecular factors regulating these processes is covered, including from a comparative biology perspective.
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