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SIX2 和 CITED1 是肾祖细胞自我更新的标志物,在肾母细胞瘤的原始成分中仍然活跃。

SIX2 and CITED1, markers of nephronic progenitor self-renewal, remain active in primitive elements of Wilms' tumor.

机构信息

Department of Pediatric Surgery, Monroe Carell Jr Children's Hospital at Vanderbilt, Nashville, Tennessee, USA.

出版信息

J Pediatr Surg. 2012 Jun;47(6):1239-49. doi: 10.1016/j.jpedsurg.2012.03.034.

Abstract

PURPOSE

SIX2 and CITED1 are transcriptional regulators that specify self-renewing nephronic progenitor cells of the embryonic kidney. We hypothesized that SIX2, which promotes and maintains this stem cell population, and CITED1 remain active in Wilms' tumor (WT).

METHODS

To evaluate expression domains and the pathogenic significance of SIX2 and CITED1 across WT, the Children's Oncology Group provided 40 WT specimens of stages I to IV (n = 10 per stage), which were enriched for unfavorable histology (n = 20) and treatment failure (relapse or death, n = 20). SIX2 and CITED1 protein expression was evaluated qualitatively (immunohistochemistry) and quantitatively (Western blot, or WB). Gene transcription was estimated using quantitative real-time polymerase chain reaction (qRT-PCR).

RESULTS

SIX2 was visualized by immunohistochemistry in 36 (94.7%) of 38 specimens. Protein and messenger RNA expression of SIX2 were quantitatively similar across all stages of disease (P = .48 WB; P = 0.38 qPCR), in favorable or unfavorable histology (P = 0.51 WB; P = 0.58 qPCR), and in treatment failure or success (P = 0.86 WB; P = 0.49 qPCR). Although CITED1 expression paralleled SIX2 qualitatively, no quantitative correlation between SIX2 and CITED1 expression was observed (Spearman correlation coefficient, 0.28; P = 0.08). As in the fetal kidney, overlapping, but also distinct, WT cellular expression domains were observed between SIX2 and CITED1.

CONCLUSION

SIX2 and CITED1 remain active across all disease characteristics of WT. Activity of these genes in WT potentially identifies a population of self-renewing cancer cells that exhibit an embryonic, stemlike phenotype. Taken together, these transcriptional regulators may be fundamental to WT cellular self-renewal and may represent targets for novel therapies that promote terminal differentiation.

摘要

目的

SIX2 和 CITED1 是转录调节因子,它们特异性地决定胚胎肾的自我更新肾祖细胞。我们假设,促进和维持这种干细胞群体的 SIX2 和 CITED1 在肾母细胞瘤(WT)中仍然活跃。

方法

为了评估 SIX2 和 CITED1 在 WT 中的表达域和发病意义,儿童肿瘤学组提供了 40 例 I 期至 IV 期 WT 标本(n = 10/期,各期均有 10 例),其中富集了不良组织学(n = 20)和治疗失败(复发或死亡,n = 20)。通过免疫组织化学(免疫组化)定性评估 SIX2 和 CITED1 蛋白的表达,并通过 Western blot(WB)或定量(WB)定量评估基因转录。使用实时定量聚合酶链反应(qRT-PCR)估计基因转录。

结果

38 例标本中的 36 例(94.7%)可见 SIX2 的免疫组织化学。SIX2 的蛋白和信使 RNA 表达在疾病的所有阶段(P =.48 WB;P = 0.38 qPCR)、良好或不良组织学(P = 0.51 WB;P = 0.58 qPCR)、治疗成功或失败(P = 0.86 WB;P = 0.49 qPCR)中均相似。虽然 CITED1 的表达与 SIX2 定性一致,但 SIX2 和 CITED1 之间的表达没有定量相关性(Spearman 相关系数,0.28;P = 0.08)。与胎儿肾脏一样,在 SIX2 和 CITED1 中观察到重叠但也不同的 WT 细胞表达域。

结论

SIX2 和 CITED1 在 WT 的所有疾病特征中仍然活跃。这些基因在 WT 中的活性可能识别出自我更新的癌细胞群体,其表现出胚胎样、干细胞样表型。总的来说,这些转录调节因子可能是 WT 细胞自我更新的基础,可能成为促进终末分化的新疗法的靶点。

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