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磷酸化-mTOR 在转移性 SDHB 副神经节瘤中没有上调。

Phospho-mTOR is not upregulated in metastatic SDHB paragangliomas.

机构信息

Department of Internal Medicine, VA North Texas Health Care System, University of Texas Southwestern Medical Center, Dallas, TX 75235, USA.

出版信息

Eur J Clin Invest. 2013 Sep;43(9):970-7. doi: 10.1111/eci.12127. Epub 2013 Jul 26.

Abstract

BACKGROUND

Pheochromocytomas (PCCs)/paragangliomas (PGLs) are neuroendocrine tumours that may cause arrhythmia and death if untreated. Treatment for patients with metastatic tumours is lacking. As new PCC/PGL susceptibility genes are discovered that are associated with the mTOR pathway, treatment targets focusing on this pathway are being intensively explored.

DESIGN

Twenty-one human PCC/PGLs were analysed from two tertiary care centres. Immunohistochemistry (IHC) analysis was performed for phospho-mTOR (pmTOR), phospho-S6K (pS6K), phosphoinositide 3-kinase (PI3K), phospho-4EBP1 (p4EBP1), HIF1α and MIB-1 in 6 metastatic SDHB PCC/PGLs, 15 nonmetastatic PCC/PGLs, (including 1 TMEM127 PCC and 1 nonmetastatic SDHB PGL) and 6 normal adrenal medullas. The product of the intensity of stain and percentage of cells stained was calculated as an H score.

RESULTS

Using a two-sample t-test and paired t-test, pmTOR and pS6K had significantly higher H scores in nonmetastatic PCC/PGLs than in metastatic SDHB PCC/PGLs. HIF1α had significantly higher H scores in metastatic SDHB PCC/PGLs compared with nonmetastatic PCC/PGLs and normal adrenal medulla. No difference in H scores was seen with p4EBP1, PI3K and MIB-1 when comparing metastatic SDHB PCC/PGLs and nonmetastatic PCC/PGLs. Significantly higher difference in pS6K was seen in normal adrenal medullas compared to nonmetastatic PCC/PGLs and metastatic SDHB PCC/PGLs.

CONCLUSION

The present results suggest that the use of mTOR inhibitors alone for metastatic SDHB PCC/PGLs may not achieve good therapeutic efficacy in patients.

摘要

背景

嗜铬细胞瘤(PCCs)/副神经节瘤(PGLs)是神经内分泌肿瘤,如果不治疗可能会导致心律失常和死亡。转移性肿瘤患者的治疗方法尚缺乏。随着新的 PCC/PGL 易感性基因被发现与 mTOR 通路相关,针对该通路的治疗靶点正在被深入探索。

设计

从两个三级护理中心分析了 21 个人类 PCC/PGL。对 6 例转移性 SDHB PCC/PGL、15 例非转移性 PCC/PGL(包括 1 例 TMEM127 PCC 和 1 例非转移性 SDHB PGL)和 6 例正常肾上腺髓质进行了磷酸化 mTOR(pmTOR)、磷酸化 S6K(pS6K)、磷酸肌醇 3-激酶(PI3K)、磷酸化 4EBP1(p4EBP1)、HIF1α 和 MIB-1 的免疫组化(IHC)分析。通过计算染色强度和染色细胞百分比的乘积来计算 H 评分。

结果

使用两样本 t 检验和配对 t 检验,非转移性 PCC/PGL 的 pmTOR 和 pS6K 的 H 评分明显高于转移性 SDHB PCC/PGL。与非转移性 PCC/PGL 和正常肾上腺髓质相比,转移性 SDHB PCC/PGL 的 HIF1α 的 H 评分明显更高。比较转移性 SDHB PCC/PGL 和非转移性 PCC/PGL 时,p4EBP1、PI3K 和 MIB-1 的 H 评分无差异。与非转移性 PCC/PGL 和转移性 SDHB PCC/PGL 相比,正常肾上腺髓质的 pS6K 差异明显更高。

结论

目前的结果表明,单独使用 mTOR 抑制剂治疗转移性 SDHB PCC/PGL 可能无法在患者中获得良好的治疗效果。

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