Breast metastatic tumors in lung can be substituted by lung-derived malignant cells transformed by alternative splicing H19 lncRNA.

Jin Biao Xu, Jun Cao, Jin Xia, Ying Zhu, Yi He, Ming Guo Cao, Bing Mu Fang, Jean Paul Thiery, Wu Zhou
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Abstract

Metastasis accounts for most cancer-associated deaths; yet, this complex process remains poorly understood, particularly the relationship between distant metastasis and primary site-derived cells. Here, we modified the classical MMTV-PyMT breast carcinoma model to trace the fate of mammary-derived carcinoma cells. We show that within the lung, when the metastatic breast carcinoma cells are conditionally depleted, transformed lung epithelial cells generate new metastases. Metastatic breast carcinoma cells transmit H19 long noncoding (lnc) RNA to lung epithelial cells through exosomes. SF3B1 bearing mutations at arginine-625 alternatively splices H19 lncRNA in lung epithelial cells, which selectively acts like a molecular sponge to sequester let-7a and induces Myc upregulation. Under the conditional elimination of primary site-derived breast carcinoma cells, lung malignant cells expressing the mutated SF3B1 splice variant dominate the newly created tumors. Our study suggests that these new carcinoma cells originating from within the colonized organ can replace the primary site-derived malignant cells whenever their expansion is abrogated using an inducible diphtheria toxin receptor in our designed system. These findings should call for a better understanding of metastatic tumors with the specific origin during cancer metastasis.

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乳腺肺转移瘤可被选择性剪接H19 lncRNA转化的肺源性恶性细胞替代。
转移是大多数癌症相关死亡的原因;然而,这个复杂的过程仍然知之甚少,特别是远处转移和原发部位来源细胞之间的关系。在这里,我们修改了经典的MMTV-PyMT乳腺癌模型,以追踪乳腺源性癌细胞的命运。我们发现,在肺内,当转移性乳腺癌细胞被有条件地耗尽时,转化的肺上皮细胞产生新的转移灶。转移性乳腺癌细胞通过外泌体将H19长链非编码(lnc) RNA传递到肺上皮细胞。携带精氨酸-625突变的SF3B1在肺上皮细胞中选择性地剪接H19 lncRNA,其选择性地像分子海绵一样隔离et-7a并诱导Myc上调。在原发部位源性乳腺癌细胞有条件消除的情况下,表达突变SF3B1剪接变异体的肺恶性细胞在新生肿瘤中占主导地位。我们的研究表明,在我们设计的系统中,当使用诱导白喉毒素受体消除原发部位衍生的恶性细胞的增殖时,这些来自定植器官内的新癌细胞可以取代原发部位衍生的恶性细胞。这些发现应该呼吁更好地了解转移性肿瘤在癌症转移过程中的特定起源。
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