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体内局部应用后光敏剂苯并卟啉衍生物在人子宫内膜中的摄取情况。

Uptake of the photosensitizer benzoporphyrin derivative in human endometrium after topical application in vivo.

作者信息

Hornung R, Fehr M K, Tromberg B J, Major A, Krasieva T B, Berns M W, Tadir Y

机构信息

Beckman Laser Institute and Medical Clinic, University of California Irvine, 1002 Health Sciences Road East, Irvine, CA 92612, USA.

出版信息

J Am Assoc Gynecol Laparosc. 1998 Nov;5(4):367-74. doi: 10.1016/s1074-3804(98)80049-2.

DOI:10.1016/s1074-3804(98)80049-2
PMID:9782140
Abstract

STUDY OBJECTIVE

To determine both the time leading to maximum endometrial drug uptake and distribution of the photosensitizer benzoporphyrin derivative-monoacid ring A (BPD-MA) after intrauterine instillation (Canadian Task Force classification ).

DESIGN

Assessment of histology specimens (Canadian Task Force classification I).

SETTING

University-based facility.

PATIENTS

Twenty-two women scheduled for hysterectomy.

INTERVENTIONS

We instilled 1.5 ml of a 2 mg/ml of BPD-MA-Hyskon solution into the uterine cavity of 22 women before hysterectomy. The fluorescence induced was measured by fluorescence microscopy on frozen sections of uterine samples from 20 of 22 patients. Systemic uptake of BPD-MA was determined in plasma of six patients by spectrofluorometry.

MEASUREMENTS AND MAIN RESULTS

The BPD-MA-induced fluorescence was maximum 1 hour after instillation, with significantly higher uptake in endometrial glands than in underlying stroma. Hormonal endometrial stimulation correlated with fluorescence intensity: atrophy < secretory phase < proliferative phase. Strongest fluorescence was seen in endometrial cancer. Drug uptake by endometrial glands was found at a depth of 2 mm from the surface. Systemic uptake of BPD-MA was under the detection level of 2 ng/ml after application.

CONCLUSION

Fluorescence in human endometrial glands suggests that selective destruction of human endometrium with photodynamic therapy may be possible 1 hour after topical application of BPD-MA for benign and malignant lesions. No systemic drug uptake, side effects, or major technical difficulties were detected. Limited penetration of the drug and selective uptake by endometrial glands provided a high degree of safety for endometrial ablation.

摘要

研究目的

确定子宫内滴注光敏剂苯并卟啉衍生物单酸环A(BPD-MA)后达到最大子宫内膜药物摄取量的时间以及其分布情况(加拿大工作组分类)。

设计

组织学标本评估(加拿大工作组分类I)。

地点

大学附属医院。

患者

22名计划进行子宫切除术的女性。

干预措施

在22名女性子宫切除术前,向其子宫腔内滴注1.5毫升浓度为2毫克/毫升的BPD-MA-Hyskon溶液。通过荧光显微镜对22名患者中20名患者的子宫样本冷冻切片进行荧光测量。通过荧光分光光度法测定6名患者血浆中BPD-MA的全身摄取情况。

测量指标及主要结果

滴注后1小时BPD-MA诱导的荧光最强,子宫内膜腺体中的摄取量明显高于其下方的基质。子宫内膜的激素刺激与荧光强度相关:萎缩期<分泌期<增殖期。子宫内膜癌中荧光最强。在距表面2毫米深处发现子宫内膜腺体对药物有摄取。给药后BPD-MA的全身摄取量低于2纳克/毫升的检测水平。

结论

人体子宫内膜腺体中的荧光表明,在局部应用BPD-MA 1小时后,光动力疗法有可能对良性和恶性病变的人体子宫内膜进行选择性破坏。未检测到全身药物摄取、副作用或重大技术困难。药物的有限渗透和子宫内膜腺体的选择性摄取为子宫内膜消融提供了高度的安全性。

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