Hernández Silvia, Font-Tello Alba, Juanpere Núria, de Muga Silvia, Lorenzo Marta, Salido Marta, Fumadó Lluís, Serrano Laia, Cecchini Lluís, Serrano Sergio, Lloreta Josep
Department of Health and Experimental Sciences, Universitat Pompeu Fabra, Barcelona, Spain.
Department of Pathology, Hospital del Mar-Parc de Salut Mar-IMIM, Barcelona, Spain.
Prostate. 2016 Jun;76(9):854-65. doi: 10.1002/pros.23176. Epub 2016 Mar 9.
SLC45A3 is the second most common ERG partner in prostate cancer (PrCa). Coexisting TMPRSS2 and SLC45A3 rearrangements are found in a subset of cases, but the meaning is still unknown.
SLC45A3-ERG and TMPRSS2-ERG rearrangements and their association with ERG and PTEN expression and with clinical and pathological features have been analyzed in 80 PrCa (PSMAR-Biobank, Barcelona, Spain). ERG and PTEN mRNA were assessed by qRT-PCR; TMPRSS2-ERG and SLC45A3-ERG by RT-PCR, FISH, and direct sequencing; and ERG expression by IHC. The endpoints were Gleason score (GS), stage, and PSA progression-free survival.
Single TMPRSS2-ERG was found in 51.6% GS ≤ 7 and 22.2% GS ≥ 8 tumors (P = 0.027). SLC45A3-ERG was found in 25 cases, 20 of them with concurrent TMPRSS2-ERG rearrangement: 11.5% GS = 6, 22.2% GS = 7, and 50% GS ≥ 8 tumors (P = 0.013). Double rearrangements were associated with higher levels of ERG mRNA (P = 0.04). Double rearrangement plus PTEN loss was detected in 0% GS = 6; 14.7% GS = 7, and 29.4% GS ≥ 8 tumors (P = 0.032). Furthermore, this triple change was present in 19.2% stage T3-4 but not in any of stage T2 tumors (P = 0.05). No relationship was found with PSA progression-free survival.
Single TMPRSS2-ERG translocation is associated with low grade PrCa. Subsequent development of SLC45A3-ERG results in higher ERG expression. The combination of double rearrangement plus PTEN loss, according to our series, is never found in low grade, low stage tumors. These findings could be potentially useful in therapeutic decision making in PrCa. Tumors with combined TMPRSS2-ERG/SLC45A3-ERG fusions plus PTEN loss should be excluded from watchful waiting and are candidates for intensive therapy. Prostate 76:854-865, 2016. © 2016 Wiley Periodicals, Inc.
SLC45A3是前列腺癌(PrCa)中第二常见的ERG融合伴侣。在一部分病例中发现了共存的TMPRSS2和SLC45A3重排,但其意义仍不明确。
对80例PrCa(PSMAR生物样本库,西班牙巴塞罗那)进行了SLC45A3-ERG和TMPRSS2-ERG重排及其与ERG和PTEN表达以及临床和病理特征的相关性分析。通过qRT-PCR评估ERG和PTEN mRNA;通过RT-PCR、FISH和直接测序评估TMPRSS2-ERG和SLC45A3-ERG;通过免疫组化评估ERG表达。观察终点为Gleason评分(GS)、分期和无PSA进展生存期。
在GS≤7的肿瘤中,51.6%发现单一TMPRSS2-ERG;在GS≥8的肿瘤中,22.2%发现单一TMPRSS2-ERG(P = 0.027)。25例发现SLC45A3-ERG,其中20例同时存在TMPRSS2-ERG重排:GS = 6的肿瘤中为11.5%,GS = 7的肿瘤中为22.2%,GS≥8的肿瘤中为50%(P = 0.013)。双重重排与更高水平的ERG mRNA相关(P = 0.04)。在GS = 6的肿瘤中,0%检测到双重重排加PTEN缺失;在GS = 7的肿瘤中,14.7%检测到;在GS≥8的肿瘤中,29.4%检测到(P = 0.032)。此外,这种三联改变在19.2%的T3-4期肿瘤中存在,但在任何T2期肿瘤中均未发现(P = 0.05)。未发现与无PSA进展生存期相关。
单一TMPRSS2-ERG易位与低级别PrCa相关。SLC45A3-ERG的后续发生导致更高的ERG表达。根据我们的系列研究,双重重排加PTEN缺失的组合在低级别、低分期肿瘤中从未发现。这些发现可能对PrCa的治疗决策有潜在帮助。具有TMPRSS2-ERG/SLC45A3-ERG融合加PTEN缺失组合的肿瘤应排除在密切观察之外,是强化治疗的候选对象。《前列腺》76:854 - 865,2016。©2016威利期刊公司
