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低剂量和高剂量碘-131给药后大鼠甲状腺组织中细胞死亡途径及凋亡-昏迷效应关系的评估

Evaluation of the cell death pathway and apoptosis-stunning effect relationship after low- and high-dose I-131 administrations in rat thyroid tissue.

作者信息

Turgut Bulent, Babul Aydan, Ozdemir Ozturk, Erselcan Taner

机构信息

Department of Nuclear Medicine, Cumhuriyet University, School of Medicine, Sivas, Turkey.

出版信息

Cancer Biother Radiopharm. 2006 Aug;21(4):342-51. doi: 10.1089/cbr.2006.21.342.

Abstract

OBJECTIVES

This study had two aims; (1) to describe the cell death pathway (apoptosis or necrosis) induced by a low and high dose of radioiodine (I-131) in rat thyroid tissue in in vivo conditions and (2) to determine the role of apoptosis in the development of "stunning effect" in the thyroid tissue with low and high doses of I-131 application.

DESIGN

The experimental group consisted of 18 rats; low and high I- 131 doses with a 1-week interval were administered to this group. At first, low doses were injected intraperitoneally (i.p.) (net injected dose was 51.54 +/- 8.6 microCi). After 1 week of the low-dose injection, high doses were also injected (net injected dose was 934.9 +/- 211.8 microCi). Thyroidal I-131 uptakes for both low- and high-dose applications were calculated by using a gamma camera after 24 hours of injections. Immediately after the uptake calculation, thyroid tissues were resected. A control group of 10 rats was also included in the study; in this group, I-131 was not administered. Thyroid tissues of this group rats were also resected. DNA was extracted from thyroid tissues, and damage was examined with the "DNA ladder by agaroz gel electrophoresis."

RESULTS

Thyroidal I-131 uptakes were calculated as 11.3% +/- 3.6% and 9.8% +/- 5.3% at the 24th hour after low- and high-dose I-131 applications, respectively. When the low- and high-dose uptake values were compared for each rat; a significant relationship was not found between thyroidal uptakes and injected low and high doses of I-131. When the chromosome images were examined, there was healthy DNA appearance in 1 rat; in 4 rats, only necrotic hyperfragmentations were observed; in 9 rats, both apoptotic specific fragmentations and necrotic hyperfragmentations were observed; and in 4 rats, apoptosis, necrosis, and healthy DNA appearances were seen together. In none of the rats, specific fragmentations concordant only with apoptosis was found. When the thyroidal uptake alterations were taken into consideration, significant difference was not found between first and second uptake calculations (p = 0.28). No significant relationship was also observed between thyroidal uptake alterations and apoptosis-necrosis-healthy DNA findings. Additionally, when we take into consideration the DNA results of only 13 of the rats that had reduced thyroidal uptake, a significant relationship could also not be observed between reduced uptake and apoptotic, necrotic, or healthy tissue findings. Interestingly, apoptotic and necrotic tissue or only necrotic, tissue findings were observed in the other 5 rats which had increased thyroidal uptake.

CONCLUSIONS

Following I-131 administration, two types of cell death--both apoptosis and necrosis findings--have been observed in most of the rats. We think that the decreased uptake values are because of the probable stunning effect in thyroid tissue. We also investigated whether the stunning effect is related to apoptosis. According to our results, it can be concluded that the stunning effect is not related to tissue damage, cell decrease, or cell death. Alternatively, we think that this can be related to a radiation-induced reduction of iodine uptake/metabolism or a modified iodine transport mechanism. For further in vivo studies, this experimental model using normal rat thyroid tissue may be useful in investigating the cell death pathways induced by I-131 and its probable roles in the development of the stunning phenomenon.

摘要

目的

本研究有两个目的;(1)描述在体内条件下低剂量和高剂量放射性碘(I - 131)诱导大鼠甲状腺组织的细胞死亡途径(凋亡或坏死),以及(2)确定在低剂量和高剂量应用I - 131时,凋亡在甲状腺组织“顿抑效应”发展中的作用。

设计

实验组由18只大鼠组成;该组大鼠以1周的间隔给予低剂量和高剂量的I - 131。首先,腹腔注射低剂量(净注射剂量为51.54±8.6微居里)。低剂量注射1周后,再注射高剂量(净注射剂量为934.9±211.8微居里)。注射24小时后,使用γ相机计算低剂量和高剂量应用时甲状腺对I - 131的摄取量。摄取量计算完成后,立即切除甲状腺组织。研究中还纳入了10只大鼠的对照组;该组未给予I - 131。该组大鼠的甲状腺组织也被切除。从甲状腺组织中提取DNA,并通过“琼脂糖凝胶电泳DNA梯带”检测损伤情况。

结果

低剂量和高剂量I - 131应用后第24小时,甲状腺对I - 131的摄取量分别计算为11.3%±3.6%和9.8%±5.3%。比较每只大鼠的低剂量和高剂量摄取值时;未发现甲状腺摄取量与注射的低剂量和高剂量I - 131之间存在显著关系。检查染色体图像时,1只大鼠的DNA外观正常;4只大鼠仅观察到坏死性超片段化;9只大鼠同时观察到凋亡特异性片段化和坏死性超片段化;4只大鼠同时出现凋亡、坏死和正常DNA外观。在任何一只大鼠中,均未发现仅与凋亡一致的特异性片段化。考虑甲状腺摄取变化时,首次和第二次摄取量计算之间未发现显著差异(p = 0.28)。甲状腺摄取变化与凋亡 - 坏死 - 正常DNA结果之间也未观察到显著关系。此外,当仅考虑甲状腺摄取降低的13只大鼠的DNA结果时,摄取降低与凋亡、坏死或正常组织结果之间也未观察到显著关系。有趣的是,在另外5只甲状腺摄取增加的大鼠中观察到凋亡和坏死组织或仅坏死组织。

结论

给予I - 131后,大多数大鼠中观察到两种类型的细胞死亡——凋亡和坏死表现。我们认为摄取值降低是由于甲状腺组织可能出现的顿抑效应。我们还研究了顿抑效应是否与凋亡有关。根据我们的结果,可以得出结论,顿抑效应与组织损伤、细胞减少或细胞死亡无关。或者,我们认为这可能与辐射诱导的碘摄取/代谢降低或碘转运机制改变有关。对于进一步的体内研究,使用正常大鼠甲状腺组织的这个实验模型可能有助于研究I - 131诱导的细胞死亡途径及其在顿抑现象发展中的可能作用。

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