局部丝裂霉素C和辐射诱导结膜dna多倍体

O. Cartsburg, C. Kallen, J. Hillenkamp, R. Sundmacher, N. Pomjanski, A. Böcking
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引用次数: 13

摘要

非典型细胞改变常发生在外用丝裂霉素C (MMC)和/或放射治疗癌前或恶性结膜瘤后。结膜上皮的这些反应性、非肿瘤性改变可能是鉴别诊断的问题。我们的目的是通过DNA图像细胞术研究MMC和放射治疗后结膜上皮细胞核DNA分布的变化。方法:对13例(13眼)鳞状细胞癌患者和6例(6眼)原位结膜恶性黑色素瘤患者在治疗前、治疗中及治疗后进行结膜刷涂片。患者分别接受MMC滴剂(0.02%或0.04%)单独治疗(n=12)、放射治疗(n=3)或两者同时治疗(n=4)。首先,对获得的毛刷涂片进行细胞学评价。其次,在Feulgen抑制后,使用AutoCyte - QUIC - DNA®工作站测定反应改变细胞的DNA含量。结果:我们在所有患者中观察到整倍体DNA -多倍体和细胞形态学变化(19/19)。我们认为这些改变是对治疗的反应。4例患者在4c和15例患者在8c时显示出最大的DNA - stemline。在MMC滴注和/或放疗期间和之后观察到这种效应,在平均随访22.5个月后,94%的患者保持稳定(标准差15.4)。在5个病例中,图像细胞术还显示DNA -茎系非整倍体是肿瘤复发的证据。结论:DNA含量测量显示形态学可疑但良性的鳞状细胞整倍体多倍体化,这是众所周知的局部化疗和/或放疗后继发形态学变化的生物学相关性。DNA -图像-细胞术在整倍体多倍体分化中是一种有用的工具,作为治疗和肿瘤复发后反应性细胞变化的标志。
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Topical Mitomycin C and Radiation Induce Conjunctival DNA-Polyploidy
Introduction: Atypical cell changes often occur following treatment of premalignant or malignant conjunctival neoplasias with topical mitomycin C (MMC) and/or radiation. These reactive, non‐neoplastic alterations of the conjunctival epithelium can be a differential diagnostic problem. Our aim was to investigate changes in the nuclear DNA‐distribution of conjunctival epithelial cells after MMC‐ and radiation therapy by DNA‐image‐cytometry. Methods: Conjunctival brush smears were obtained from 13 patients (13 eyes) with squamous cell carcinomas and six patients (6 eyes) with conjunctival malignant melanomas in situ before, during and after treatment. The patients were treated with MMC‐drops (0.02% or 0.04%) alone (n=12), with radiation therapy (n=3) or both (n=4). At first, the obtained brush smears were evaluated by cytology. Secondly, after Feulgen restaining, the DNA content of reactively changed cells was determined using the AutoCyte‐QUIC‐DNA® workstation. Results: We observed euploid DNA‐polyploidy and cytomorphological changes in all patients (19/19). We considered these alterations as reactive to treatment. Four patients showed their greatest DNA‐stemline at 4c and 15 patients at 8c. This effect was observed during and following MMC‐drops and/or radiation and remained stable in 94% of all patients after a mean follow‐up of 22.5 months (SD 15.4). In five cases image cytometry additionally demonstrated DNA‐stemline aneuploidy as an evidence of tumor recurrence. Conclusion: Measurements of DNA‐content revealed euploid polyploidisation of morphological suspicious but benign squamous cells which is the biologic correlate of well known secondary morphologic changes following topical chemotherapy and/or radiation. DNA‐image‐cytometry is a useful tool in the differention of euploid polyploidization as a sign of reactive cell changes following treatment and tumor recurrences.
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