首页> 外文期刊>Journal of Endocrinological Investigation: Official Journal of the Italian Society of Endocrinology >Immunohistochemical localization and quantitative expression of somatostatin receptors in normal human spleen and thymus: Implications for the in vivo visualization during somatostatin receptor scintigraphy
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Immunohistochemical localization and quantitative expression of somatostatin receptors in normal human spleen and thymus: Implications for the in vivo visualization during somatostatin receptor scintigraphy

机译:正常人脾脏和胸腺中生长抑素受体的免疫组织化学定位和定量表达:对生长抑素受体闪烁显像的体内可视化意义

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Background: [ 111In-DTPA-D-Phe 1]-octreotide scintigraphy allows the visualization of SRIF receptor (SSR)-expressing tumors, including thymic tumors, and normal tissues. While the spleen is clearly visualized, the thymus is not depicted, although both contain SSR. Aim: We evaluated whether the heterogeneity, the type, and the amount of SSR might explain this contrasting finding. Materials, methods, and results: By ligand-binding the number of [ 125I-Tyr 11]-SRIF-14 binding sites resulted comparable between the two tissues, whereas the number of [ 125I-Tyr 3]-octreotide sites was significantly higher in the spleen (p0.001). Quantitative RT-PCR showed a significantly higher expression of sst 2A mRNA in the spleen, whereas a significantly higher expression of SRIF and sst 3 in the thymus. The highest density of sst 2A in the spleen is in line with the in vivo uptake of [ 111In-DTPA-D-Phe 1]-octreotide, which is considered a sst2-preferring ligand. The specificity is confirmed by the evidence that in vivo [ 111In-DT-PA-D-Phe 1]-octreotide uptake can be abolished during chronic administration of "cold" octreotide. Immunohistochemistry confirmed a preferential expression of sst 2A on microenvironmental cells and of sst 3 on lymphoid cells. Conclusions: The heterogeneity of SSR expression and the higher SRIF content explain the lack of thymus visualization during scintigraphy, whereas thymic tumors, which do not express SRIF, are visualized. Apart from the affinity of the radioligand, also the efficacy of the internalization is crucial for the in vivo uptake, and both heterogeneity and SRIF content affect this process. These observations might have an important impact when interpretating in vivo visualization of SSR-positive lesions, and when treatment with novel SRIF analogs is considered.
机译:背景:[111In-DTPA-D-Phe 1]-奥曲肽闪烁显像术可以观察到表达SRIF受体(SSR)的肿瘤,包括胸腺瘤和正常组织。尽管脾脏清晰可见,但胸腺并未显示,尽管它们都包含SSR。目的:我们评估了SSR的异质性,类型和数量是否可以解释这一对比发现。材料,方法和结果:通过配体结合,两个组织之间[125I-Tyr 11] -SRIF-14结合位点的数量可比,而[125I-Tyr 3]-奥曲肽位点的数量明显更高。脾脏(p <0.001)。定量RT-PCR显示,脾脏中sst 2A mRNA的表达明显较高,而胸腺中SRIF和sst 3的表达明显较高。脾脏中sst 2A的最高密度与[111In-DTPA-D-Phe 1]-奥曲肽的体内摄取一致,后者被认为是sst2优先配体。通过在长期服用“冷”奥曲肽的过程中可以消除体内[111In-DT-PA-D-Phe 1]-奥曲肽的摄取,证实了特异性。免疫组织化学证实,sst 2A在微环境细胞上优先表达,sst 3在淋巴样细胞上优先表达。结论:SSR表达的异质性和较高的SRIF含量解释了闪烁显像过程中胸腺可视化的缺乏,而未表达SRIF的胸腺肿瘤则可见。除了放射性配体的亲和力外,内化作用的有效性对于体内摄取也至关重要,异质性和SRIF含量均会影响该过程。在解释SSR阳性病变的体内可视化以及考虑使用新型SRIF类似物进行治疗时,这些观察结果可能会产生重要影响。

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