髓系来源的抑制细胞群体的扩增在γ疱疹病毒促进乳腺癌转移中不起作用。
An expanded myeloid derived suppressor cell population does not play a role in gammaherpesvirus-exacerbated breast cancer metastases.
机构信息
Department of Biology, University of North Carolina at Charlotte, 9201 University City Blvd, Charlotte, North Carolina, USA.
出版信息
Infect Agent Cancer. 2012 Sep 4;7(1):22. doi: 10.1186/1750-9378-7-22.
BACKGROUND
Mice latently infected with murine gammaherpesvirus 68 (HV-68) and transplanted with 4 T1 breast cancer cells developed exacerbated metastatic lesions when compared to controls. The mechanisms responsible for this viral-exacerbated disease were not clear. The ability of HV-68 infection to induce S100A8 and S100A9 production and to expand a population of CD11b+Gr-1+ cells suggested that increased numbers, or activity, of viral-expanded myeloid derived suppressor cells (MDSCs) might contribute to HV-68-associated metastatic breast cancer in this model. We questioned whether mock or HV-68 infected mice with significant breast cancer might have differences in the number and/or activity of MDSCs.
METHODS
Myeloid-derived macrophages and dendritic cells were isolated from normal mice and cultured in vitro with HV-68 to assess S100A8 and S100A9 mRNA and protein expression. In vivo studies were performed using groups of mice that were mock treated or infected with HV-68. After viral latency was established, 4 T1 breast cancer cells were transplanted in mice. When primary breast tumors were present mice were euthanized and cells isolated for phenotyping of myeloid cell populations using FACS, and for ex vivo analysis of suppressor activity. Serum from these animals was also collected to quantify S100A8 and S100A9 levels.
RESULTS
In vitro studies demonstrated that direct exposure of myeloid cells to HV-68 did not induce increased expression of S100A8 or S100A9 mRNAs or secreted protein. HV-68 infected mice with metastatic breast cancer disease had no increases in S100A8/A9 levels and no significant increases in the numbers or activation of CD11b+Gr-1+MDSCs when compared to mock treated mice with breast cancer.
CONCLUSIONS
Together these studies are consistent with the notion that expanded myeloid derived suppressor cells do not play a role in gammaherpesvirus-exacerbated breast cancer metastases. The mechanisms responsible for HV-68 induced exacerbation of metastatic breast cancer remain unclear.
背景
与对照组相比,潜伏感染鼠γ疱疹病毒 68(HV-68)并移植了 4T1 乳腺癌细胞的小鼠发展出了更严重的转移性病变。导致这种病毒加重疾病的机制尚不清楚。HV-68 感染诱导 S100A8 和 S100A9 产生并扩增 CD11b+Gr-1+细胞群的能力表明,病毒扩增的髓源性抑制细胞(MDSC)数量增加或活性增加可能导致该模型中与 HV-68 相关的转移性乳腺癌。我们质疑患有大量乳腺癌的假手术或 HV-68 感染小鼠是否在 MDSC 的数量和/或活性上存在差异。
方法
从正常小鼠中分离出髓样衍生的巨噬细胞和树突状细胞,并在体外与 HV-68 共培养,以评估 S100A8 和 S100A9 mRNA 和蛋白的表达。使用假手术或 HV-68 感染的小鼠进行体内研究。在病毒潜伏建立后,将 4T1 乳腺癌细胞移植到小鼠中。当原发性乳腺癌存在时,处死小鼠并分离细胞,使用 FACS 对髓样细胞群进行表型分析,并进行体外抑制活性分析。还收集这些动物的血清以定量 S100A8 和 S100A9 水平。
结果
体外研究表明,髓样细胞直接暴露于 HV-68 不会诱导 S100A8 或 S100A9 mRNA 或分泌蛋白的表达增加。与患有乳腺癌的假手术小鼠相比,患有转移性乳腺癌疾病的 HV-68 感染小鼠的 S100A8/A9 水平没有增加,并且 CD11b+Gr-1+MDSC 的数量或激活也没有显著增加。
结论
这些研究一致表明,扩张的髓源性抑制细胞在γ疱疹病毒加重的乳腺癌转移中不起作用。导致 HV-68 诱导的转移性乳腺癌加重的机制仍不清楚。
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