Circulating tumor cells(CTCs)in breast cancer:a diagnostic tool for prognosis and molecular analysis

Metastatic breast cancer （MBC） is characterized by a combination of tumor growth, proliferation and metastatic progression and is typically managed with palliative intent. The benefit of standard systemic therapies is relatively limited and the disease is considered incurable suggesting the need to investigate the biological drivers of the various phases of the metastatic process in order to improve the selection of molecularly driven therapies. The detection, enumeration and molecular analysis of circulating tumor cells （CTCs） provide an intriguing opportunity to advance this knowledge. CTCs enumerated by the Food and Drugs Administration-cleared CellSearchTM system are an independent prognostic factor of progression- free survival （PFS） and overall survival （OS） in MBC patients. Several published papers demonstrated the poor prognosis for MBC patients that presented basal CTC count _〉5 in 7.5 mL of blood. Therefore, the enumeration of CTCs during treatment for MBC provides a tool with the ability to predict progression of disease earlier than standard timing of anatomical assessment using conventional radiological tests. During the metastatic process cancer cells exhibit morphological and phenotypic plasticity undergoing epithelial- mesenchymal transition （EMT）. This important phenomenon is associated with down regulation of epithelial marker （e.g., EpCAM） with potential limitations in the applicability of current CTCs enrichment methods. Such observations translated in a number of investigations aimed at improving our capabilities to enumerate and perform molecular characterization of CTCs. Theoretically, the phenotypic analysis of CTCs can represent a ＂liquid＂ biopsy of breast tumor that is able to identify a new potential target against the metastatic disease and advance the development and monitoring of personalized therapies.

Circulating tumor cells isolation:the "post-EpCAM era"

Circulating tumor cells （CTCs） represent a submicroscopic fraction detached from a primary tumor and in transit to a secondary site. The prognostic significance of CTCs in metastatic cancer patients was demonstrated for the first time more than ten years ago. To date, it seems clear enough that CTCs are highly heterogeneous and dynamically change their shape. Thus, the inadequacy of epithelial cell adhesion molecule （EpCAM） as universal marker for CTCs detection seems unquestionable and alternative methods able to recognize a broader spectrum of phenotypes are definitely needed. In this review the pleiotropic functions of EpCAM are discussed in detail and the role of the molecule in the biology of CTCs is critically dissected.

Single-cell analyses of circulating tumor cells

Circulating tumor cells(CTCs) are a population of tumor cells mediating metastasis, which results in most of the cancer related deaths. The number of CTCs in the peripheral blood of patients is rare, and many platforms have been launched for detection and enrichment of CTCs. Enumeration of CTCs has already been used as a prognosis marker predicting the survival rate of cancer patients. Yet CTCs should be more potential. Studies on CTCs at single cell level may help revealing the underlying mechanism of tumorigenesis and metastasis. Though far from developed, this area of study holds much promise in providing new clinical application and deep understanding towards metastasis and cancer development.

Impact of chronic exposure to bevacizumab on EpCAM-based detection of circulating tumor cells

Background： Circulating tumor cells （CTCs） are often undetected through the immunomagnetic epithelial cell adhesion molecule （EpCAM）-based CellSearch~ System in breast and colorectal cancer （CRC） patients treated with bevacizumab （BEV）, where low CTC numbers have been reported even in patients with evidence of progression of disease. To date, the reasons for this discrepancy have not been clarified. This study was carried out to investigate the molecular and phenotypic changes in CRC cells after chronic exposure to BEV in vitro. Methods： The human CRC cell line WiDr was exposed to a clinically relevant dose of BEV for 3 months in vitro. The expression of epithelial and mesenchymal markers and EpCAM isoforms was determined by western blotting and immunofluorescence. To evaluate the impact of EpCAM variant isoforms expression on CTC enumeration by CellSearch, untreated and treated colon cancer cells were spiked into 7.5 mL of blood from a healthy donor and enumerated by CellSearch. Results： Chronic exposure of CRC cell line to BEV induced decreased expression of EpCAM 40 kDa isoform and increased expression EpCAM 42 kDa isoform, together with a decreased expression of cytokeratins （CK）, while no evidence of epithelial to mesenchymal transition （EMT） in treated cells was observed. The recovery rate of cells through CellSearch was gradually reduced in course of treatment with BEV, being 84% , 70% and 40% at l, 2 and 3 months, respectively. Conclusions： We hypothesize that BEV may prevent CellSearch from capturing CTCs through altering EpCAM isoforms.

Growth of Circulating Tumor Cell-Derived Colonies from Peripheral Blood of Melanoma Patients: Preliminary Characterization of Colony Composition

Circulating tumor cells (CTC) are rarely detected in the blood of cancer patients, even though they are a direct harbinger of eventual patient demise. We developed an innovative CTC culture technology to allow more sensitive isolation, expansion, and characterization of viable colonies from patient blood. In this assay, the entire leukocyte fraction from 10 ml of anticoagulated patient blood is placed into culture medium without any pre-selection. After 16 days in culture, CTC derived colonies are counted. As a proof-of-principle, blood samples from 58 Stage IIa-IV melanoma patients were tested. Ninety percent of these samples grew colonies. The colony numbers ranged from 0 - 308 (mean 63 ± 9.5 SEM). Ten normal volunteers had virtually no growth (mean 0.5 ± 1.4 colonies). Colonies were harvested using a micropipette for characterization. Tumor-cell containing spheroids were embedded in paraffin, sectioned, and stained with melanoma-specific mAb for histologic characterization. MITF proved to be the most consistent immunostain that identified melanoma cells in these colonies. A host-cell component in colonies was also identified using CD68 and CD43 mAb staining. Following enzymatic dissociation of colonies, a variety of immunostains were tested. Papanicolau staining proved most useful for identifying the abnormal nuclei of tumor cells. Flow cytometry could readily distinguish host and tumor cell populations based on DNA content and forward/side scatter in dissociated colonies. The stem cell marker ALDH1A1 associated with the aneuploid population, but CD45 was expressed on both diploid and aneuploid cells. The ability to repeatedly isolate CTC derived colonies from cancer patient blood samples opens the door to a novel type of long-term clinical monitoring. This novel CTC culture technology may prove useful to perform molecular characterization, assessment of treatment response, and testing of drug sensitivity and resistance in patients during treatment.

Circulating Tumor Cell Cultures as a Predictive Marker during Salvage Therapy of Refractory Merkel Cell Carcinoma with Chemotherapy and Electron Beam Radiation

Metastatic Merkel Cell carcinoma (MCC) is a highly unusual and aggressive skin cancer that presents as a small, pink to violet skin lesion and metastasizes early in its growth. Metastatic MCC is generally treated with small cell lung cancer chemotherapy regimens, because the tumor consists of neuroendocrine cells, but patients generally do not have durable responses. The pathogenesis of MCC has recently been attributed to the Merkel Cell polyoma virus. This virus activates the cellular retinoblastoma oncoprotein and cell cycle machinery, triggering continual cellular proliferation. A 77-year-old man developed extensive MCC metastases, involving more than one fourth of his scalp and numerous cervical lymph nodes. Following failure of initial chemotherapy and radiation, effective palliation was achieved by using a sequence of electron-beam radiotherapy, low dose gemcitabine, and etoposide, resulting in significant periods of tumor regression and prolonged survival. A novel circulating tumor cell (CTC) culture assay was performed on four separate clinic visits during the treatment period. Tumor colonies were cultured from the patient’s peripheral blood and CTC colony counts were correlated with clinical treatment response. Not only did the patient respond to palliative cell cycle directed chemotherapy and electron beam radiation, but we demonstrated that CTC can be cultured from peripheral blood of MCC patients and serve as a predictive marker to monitor treatment response.

Notes for developing a molecular test for the full characterization of circulating tumor cells

The proved association between the circulating tumor cell （CTC） levels and the patients＇ survival parameters has been growing interest to investigate the molecular profile of these neoplastic cells among which hide out precursors capable of initiating a new distant metastatic lesion. The full characterization of the tumor cells in peripheral blood of cancer patients is expected to be of help for understanding and （prospectively） for counteracting the metastatic process. The major hitch that is hampering the successful gaining of this result is the lack of a consensus onto standard operating procedures （SOPs） for performing what we generally define as the ＂liquid biopsy＂. Here we review the more recent acquisitions in the analysis of CTCs and tumor related nucleic acids, looking to the main open questions that are hampering their definitive employ in the routine clinical practice.

Research progress on circulating tumor cell detection in brain gliomas

Glioma,the most common primary intracranial tumor,has high morbidity and mortality.The detection of circulating tumor cells(CTCs)is an important part of the liquid biopsy of gliomas.CTCs,carrying the genetic and biological information of tumor tissue,provide a new perspective and dimension for the study of tumor metastasis,progression,chemotherapy sensitivity and drug resistance.Cerebrospinal fluid(CSF)circulates through the ventricle and spinal cord cistern,which can better maintain the original information of tumor cells compared with the complicated environments of tissues and plasma.Study on the dynamic changes of CTCs in the CSF of the central nervous system(CNS)is relatively rare.However,the analysis of CTCs in CSF can be used to guide the treatment of gliomas and reveal the patho-physiological and genetic mechanisms of tumor cell metastasis to the CSF.This paper reviews the progress in the research on CTC detection in gliomas.

Circulating cancer stem cells:the importance to select

It has been demonstrated that even localized tumors withottt chnically apparent metastasis give rise to circulating tumor cells （CTCs）. A growing number of technically diverse platforms are being developed for detecting/isolating CTCs in the circulating blood. Despite the technical challenges of isolating rare CTCs from blood, recent studies have already shown the predictive value of CTCs enumeration. Thus, it is becoming increasingly accepted that CTC numbers are linked to patients＇ outcome and may also be used to monitor treatment response and disease relapse, respectively. Further CTCs provide a non-invasive source for tumor material, ＇liquid biopsy＇, which is particularly important for patients, where no biopsy material can be obtained or where serial biopsies of the tumor, e.g., following treatment, are practically impossible. On the other hand the molecular and biological characterization of CTCs has still remained at a rather experimental stage. Future studies are necessary to define CTC heterogeneity to establish the crucial role of circulating cancer stem cells for driving metastasis, which represent a distinct subpopulation of CTCs that bear metastasis-initiating capabilities based on their sternness properties and invasiveness and thus are critical for the patients＇ clinical outcome. As compared to non-tumorigenic/metastatic bulk CTCs, circulating cancer stem cells may not only be capable of evading from the primary tumor, but also escape from immune surveillance, survive in the circulating blood and subsequently form metastases in distant organs. Thus, circulating cancer stem cells represent a subset of exclusively tumorigenic cancer stem cells characterized by their invasive characteristics and are potential therapeutic targets for preventing disease progression. To date, only a few original reports and reviews have been published focusing on circulating cancer stem cells. This review discusses the potential importance of isolating and characterizing these circulating cancer stem cells, but also highlights current technological limitations.

Interaction between circulating cancer cells and platelets:clinical implication

Metastasis is the main cause of cancer-associated mortality. During this complicated process, some cancer cells, also called circulating tumor cells （CTCs）, detach from primary sites, enter bloodstream and extravasate at metastatic site. Thrombocytosis is frequently observed in patients with metastatic cancers suggesting the important role of platelets in metastasis. Therefore this review focuses on how platelets facilitate the generation of CTCs, protect them from various host attacks, such as immune assaults, apoptosis and shear stress, and regulate CTCs intravasation/extravasation. Platelet-derived cytokines and receptors are involved in this cascade. Identification the mechanisms underlie platelet-CTCs interactions could lead to the development of new platelet-targeted therapeutic strategy to reduce metastasis.

免疫磁珠负性富集结合免疫荧光抗体技术检测卵巢癌患者外周血CTCs的方法建立和应用

目的建立基于细胞学水平的循环肿瘤细胞负性富集技术来检测卵巢上皮性癌(卵巢癌)患者外周血循环肿瘤细胞。方法体外培养卵巢癌SKOV-3细胞,按一定比例掺入到2 ml健康人外周静脉血中,应用免疫磁珠为基础的负性富集结合免疫荧光抗体技术对循环肿瘤细胞进行定量检测。评价该方法富集靶细胞的回收率,并用上述方法检测32例卵巢癌患者和10例对照者外周血中的循环肿瘤细胞。结果①在健康志愿者2 ml外周血掺入不同数目SKOV-3细胞的条件下,肿瘤细胞的回收率在64%~80%之间,掺入细胞间回归方程为Y=0.782X-1.408,相关系数为0.998。②10例对照者外周血中未检测到CK8/18+,18例卵巢癌患者的外周血中检测到CK8/18+,阳性率为56.3%(18/32,X^2=7.681,P<0.01)。③CTCs阳性与远处转移密切相关(X^2=5.776,P<0.05)。结论免疫磁珠负性富集结合免疫荧光抗体技术检测卵巢癌患者外周血循环肿瘤细胞的方法可能具有一定的临床应用价值。

检测循环肿瘤细胞(CTC)在临床肿瘤诊断和治疗中的作用

有关循环肿瘤细胞的理论已有很长时间。肿瘤转移及复发的过程均是一个循环肿瘤细胞定植生长的级连放大的瀑布反应。目前肿瘤的发现和诊断仍高度依赖于影像学及肿瘤特异性血清标志物的方法,不能及时发现肿瘤的转移和复发。基于肿瘤细胞播散理论,检测循环肿瘤细胞可更早期有效发现肿瘤的早期转移和复发。本文对文献报道的检测循环肿瘤细胞在临床肿瘤诊断和治疗中的作用进行了总结,并与目前经典的标志物和影像学进行了比较。

立体定向精准放射治疗对老年非小细胞肺癌的临床疗效及对外周血CTCs和TK1的影响

目的:探讨立体定向精准放射治疗(SBRT)对老年非小细胞肺癌(NSCLC)的临床疗效及对外周血循环肿瘤细胞(CTCs)和胸苷激酶1(TK1)的影响。方法:选取医院收治的60例NSCLC患者,依据随机数表法将其分为观察组和对照组,每组30例。观察组采用SBRT,对照组采用常规放射治疗,记录治疗期间两组不良反应发生情况,随访3年记录生存期。评估治疗前后肺功能,以及治疗前后、治疗后1年和末次随访检测外周血CTCs数目和TK1水平。结果:观察组治疗总有效率和疾病控制率分别为63.3%和86.7%,显著高于对照组的36.7%和63.3%,差异有统计学意义(x^(2)=4.267,x^(2)=4.356;P<0.05)。治疗后,观察组肺通气阻抗中的中心阻力(Rc)、周边阻力(Rp)、5 Hz的总气道阻力(R5)、20 Hz的总气道阻力(R20)和呼吸总阻抗(Zrs)指标均低于对照组,差异有统计学意义(t=4.076,t=3.429,t=3.942,t=3.083,t=3.545;P<0.05);观察组不良反应中恶心呕吐、食欲下降、皮肤瘙痒和湿疹均低于对照组,差异有统计学意义(x^(2)=4.800,x^(2)=4.444,x^(2)=4.022,x^(2)=4.356;P<0.05);观察组放射性肺炎、放射性食管炎发生率低于对照组,差异有统计学意义(x^(2)=19.631,x^(2)=10.814;P<0.05);观察组各时间点外周血CTCs数目、TK1水平均低于对照组,差异有统计学意义(F=19.834,F=15.023;P<0.05)。观察组中位生存期显著高于对照组,差异有统计学意义(x^(2)=21.280,P<0.05)。结论:SBRT对老年NSCLC安全性高,对肺损伤小,不良反应少,并能降低外周血CTCs数目和TK1水平,改善肺功能,提高近期疗效,延长生存期。

循环肿瘤细胞联合血清整合素β1对病理性乳头溢液患者乳管内恶性病变的诊断价值

目的探讨循环肿瘤细胞(CTCs)联合整合素β1(ITGβ1)对病理性乳头溢液(PND)患者乳管内恶性病变的诊断价值。方法回顾性分析2022年1月至2023年9月北京市通州区妇幼保健院及首都医科大学附属北京朝阳医院收治的212例PND患者的临床资料,根据乳管病理检查结果将研究对象分为良性病变组(187例)和恶性病变组(25例)。采用差异富集-荧光免疫染色原位杂交技术(SE-iFISH)检测PND患者CTCs数量,采用酶联免疫吸附试验检测PND患者血清ITGβ1水平。采用多因素logistic回归分析PND患者发生乳管内恶性病变的影响因素。通过受试者工作特征(ROC)曲线分析CTCs数量、血清ITGβ1水平对PND患者乳管内恶性病变的诊断效能。结果两组年龄、体质量指数(BMI)、月经状态、溢液类型、乳腺肿块比较差异有统计学意义(P<0.05)。恶性病变组CTCs数量多于良性病变组,血清ITGβ1水平高于良性病变组,差异有统计学意义(P<0.05)。多因素logistic回归分析结果显示,年龄>50岁、BMI>24 kg/m^(2)、血样溢液、较多的CTCs数量、较高的血清ITGβ1水平是PND患者发生乳管内恶性病变的独立危险因素(P<0.05)。CTCs数量、血清ITGβ1水平均具有诊断PND患者乳管内恶性病变的应用价值(P<0.05),且两项指标联合检测的诊断效能更优[AUC(95%CI)=0.961(0.925~0.983),P<0.001],灵敏度和特异度分别为96.00%、84.49%。结论CTCs数量、血清ITGβ1水平在乳管内恶性病变的PND患者体内显著升高,二者联合对PND患者乳管内恶性病变具有较好的诊断价值。

Envita’s Precision Cancer Care: 35-Fold Improvement in Response Rates

New clinical approaches are imperative beyond the widely adopted National Comprehensive Cancer Network (NCCN) guidelines, utilized by prominent cancer institutions. Cancer is the leading cause of death among individuals younger than 85 years within the United States. Despite significant technological advances, including the expenditure of hundreds of billions, treatment outcomes and overall survival have not notably improved for most types of advanced cancer over the last several decades. Over the past 24 years, Envita Medical Centers has pioneered a unique form of personalized treatment approach for late-stage and refractory cancer patients, introducing groundbreaking innovations in the field. Our integrated algorithm utilizes advanced genomics, transcriptomics, and highly tailored immunotherapy, resulting in remarkable outcome improvements. This study presents Envita’s innovative personalized treatment algorithms and examines the response outcomes of 199 late-stage cancer patients treated at Envita Medical Centers over a two-year period. Compared to standard of care and palliative chemotherapy, Envita’s treatment demonstrated a remarkable 35-fold improvement in overall response rates (Figure 1). Moreover, 88% of the patients, the majority presenting with Stage 3 or 4 cancer, experienced a 43-fold improvement in quality of life with minimal side effects, as compared to standard of care chemotherapy and palliative care. This revolutionary success is attributed to Envita’s personalized therapeutic algorithms, which incorporate customized immunotherapy. Envita’s precision care approach has also achieved a 100% better response rate compared to over 65 global chemotherapy clinical trials with more than 2700 patients. The results from this study suggest that a wider utilization of Envita’s personalized approach can significantly benefit patients with late-stage and refractory cancer.

不同手术入路对早期甲状腺乳头状癌患者术后循环肿瘤细胞水平的影响探讨

目的探讨不同手术入路对早期甲状腺乳头状癌(PTC)患者术后循环肿瘤细胞(CTCs)水平的影响。方法回顾性分析2017年12月至2022年3月南宁市第二人民医院收治的109例早期PTC患者的临床资料,其中接受传统开放手术者78例(A组),经腋窝入路腔镜甲状腺手术者14例(B组),经颏下前庭入路腔镜甲状腺手术者17例(C组)。比较三组围术期指标、术后住院时间,以及术后CTCs分型和水平差异。结果A组术中出血量、清扫淋巴结数大于B组、C组,术后拔管时间、术后住院时间长于C组,差异有统计学意义(P<0.05)。B组术后拔管时间显著长于C组(P<0.05)。三组手术时间比较差异无统计学意义(P>0.05)。三组CTCs阳性率比较差异无统计学意义(P>0.05)。三组总CTCs计数及混合型CTCs计数比较差异有统计学意义(P<0.05),其中C组术后计数水平最高。结论三种入路术式均对早期PTC取得良好的疗效,且安全性好。不同入路术式对患者术后的CTCs水平产生了一定影响,但这种差异对患者预后的影响尚需进一步验证。

基于CELLSEARCH^(TM)系统的乳腺癌循环肿瘤细胞临床研究概览

乳腺癌是女性人群常见的恶性肿瘤,检测循环肿瘤细胞(CTCs)在乳腺癌患者中的临床价值已成为近年的研究热点之一。当前CTCs的检测方法种类繁多,但方法学差异带来的异质性问题却制约了研究数据的对比与分析。较早上市的CELLSEARCHTM系统仍是目前检测CTCs的"金标准"方法,多数CTCs相关临床研究正是基于这一检测方法。因此,本文仅对基于CELLSEARCHTM系统的乳腺癌CTCs临床研究进行复习、分类与综述,以获得具有可比性的乳腺癌CTCs临床研究概览。

血清VEGF、TLR4水平及CTCs在肺癌、乳腺癌和前列腺癌骨转移中的临床意义

目的探讨血管调控因子血管内皮生长因子(VEGF)、Toll样受体4 (TLR4)联合循环肿瘤细胞(CTCs)在肺癌、乳腺癌和前列腺癌骨转移中的临床意义。方法回顾性分析吴川市人民医院肿瘤科2019年1~12月收治的100例初诊肺癌、乳腺癌及前列腺癌骨转移患者(骨转移组)的临床资料,观察不同骨转移灶数目、临床疗效及有无骨相关发生事件发生患者的VEGF、TLR4、CTCs表达水平;另选择同期我院收治的94例初诊肺癌、乳腺癌及前列腺癌无骨转移患者纳入对照组,比较骨转移组与对照组患者的VEGF、TLR4、CTCs表达水平。结果骨转移组患者的VEGF、TLR4、CTCs阳性率分别为(341.85±40.68) pg/mL、14.19±1.37、67.00%,明显高于对照组的(236.97±28.75) pg/mL、10.15±1.12、14.89%,差异均具有统计学意义(P<0.05);骨转移灶数目≥3处组患者的VEGF、TLR4、CTCs阳性率分别为(355.09±43.29) pg/mL、15.03±1.48、82.35%,明显高于骨转移灶数目<3处组的313.72±1.33、62.03%,明显低于无效组的(371.14±44.27) pg/mL、16.28±1.53、85.71%,差异均具有统计学意义(P<0.05);有骨相关事件发生组患者的VEGF、TLR4、CTCs阳性率分别为(363.03±42.26) pg/mL、15.79±1.41、79.49%,明显高于无骨相关事件发生组的(328.31±39.67) pg/mL、13.17±1.34、59.02%,差异均有统计学意义(P<0.05)。结论血管调控因子VEGF、TLR4及CTCs可用于肺癌、乳腺癌及前列腺癌骨转移的诊断、疗效和骨相关事件的评估。

奥希替尼治疗EGFR突变阳性非小细胞肺癌的疗效及对患者外周血CTC、VEGF、CA125表达的影响

目的探究奥希替尼治疗表皮生长因子(EGFR)突变阳性非小细胞肺癌(NSCLC)的疗效、不良反应及对患者外周血循环肿瘤细胞(CTC)、血管内皮生长因子(VEGF)、糖类抗原125(CA125)表达的影响。方法以83例EGFR突变阳性NSCLC患者为研究对象,根据化疗方法不同将其分为观察组(奥希替尼治疗,41例)和对照组(铂类制剂化疗,42例),均于治疗后随访1年。比较2组临床疗效及预后;观察2组治疗前后外周血CTC、VEGF、CA125表达情况;统计2组患者化疗期间毒副作用发生情况。结果观察组疾病控制率高于对照组(P<0.05)。治疗后,观察组外周血CTC值及VEGF、CA125水平低于对照组,FEV1、FEV1/FVC值大于对照组(P<0.05)。治疗后观察组生理状况、功能状况及附加关注情况评分高于对照组(P<0.05)。观察组治疗后1年生存率高于对照组,治疗期间血小板减少症发生率低于对照组(P<0.05)。结论奥希替尼治疗EGFR突变阳性NSCLC的疗效较好,可减少外周血CTC,抑制VEGF、CA125表达,并能降低毒副作用,改善生活质量。

481例恶性肿瘤患者循环肿瘤细胞(CTC)检测的回顾性分析

目的基于CellSearch平台,回顾性分析肝癌、胃癌、结直肠癌、乳腺癌、胰腺癌、肺癌、前列腺癌7类肿瘤患者循环肿瘤细胞(circulating tumor cell,CTC)数量及形态特征,探讨其临床价值。方法回顾分析复旦大学附属中山医院检验科2014年12月至2016年4月7类肿瘤患者共481例CTC检测结果,有CTC检出者回顾原始荧光检测图像,随访时间更新至2018年4月。比较7类肿瘤患者术前、术后CTC数量变化及形态特征。分析肝癌患者不同治疗阶段的CTC形态变化及其临床价值。结果术前组CTC检出率为53%～100%,术后组为0～37%,7类肿瘤术后组均有显著下降,其中乳腺癌和胃癌下降最为显著(χ2=9.12,P=0.003;χ2=5.76,P=0.016)。不同肿瘤CTC形态存在较大异质性,以肝癌和肺癌为甚。肝癌患者连续监测结果显示,不同治疗阶段的CTC数量及形态均有变化且与临床预后相关。结论 7类肿瘤术后组CTC7.5检出率显著低于术前组。在肝癌治疗监测过程中,CTC形态变化对于治疗反应及临床预后可能有一定的提示作用。