Jerry D J, Ozbun M A, Kittrell F S, Lane D P, Medina D, Butel J S
Division of Molecular Virology, Baylor College of Medicine, Houston, Texas 77030.
Cancer Res. 1993 Jul 15;53(14):3374-81.
Preneoplastic lesions in the mammary gland represent a population of cells at increased risk of progression to tumors. Because p53 is the most commonly mutated gene in human breast cancer, we sought to determine whether mutations in p53 were present in preneoplastic lesions or were acquired during progression to overt tumors. In the mouse mammary gland, hyperplastic alveolar nodules (HAN) are the most common preneoplastic lesion. Analysis of the TM series of transplantable murine HAN outgrowths and tumors allowed the status of p53 to be determined at distinct stages of mammary tumorigenesis. Alterations in the p53 gene or in the pattern of p53 protein expression were observed in all five HAN outgrowth lines examined. Altered expression of p53 protein was detected in 3 of 5 TM HAN outgrowth lines as determined by immunohistochemistry. Overexpression of nuclear p53 was detected in only a fraction of the cells (10-50%) in TM3 and TM4 HAN outgrowths, whereas in tumors that arose from TM4 HAN outgrowths, the proportion of cells overexpressing p53 protein approached approximately 100%. Despite overexpression of p53 in TM3 HAN outgrowths, no tumors have developed in this line. The TM9 outgrowth line exhibited a different pattern of p53 expression by immunohistochemistry: p53 protein was overexpressed in the cytoplasm of virtually all cells in the HAN outgrowths but was localized to the nuclei of TM9 tumor cells. Direct sequencing of p53 transcripts from tumors and cell lines revealed various genetic changes: point mutations in exons 4 and 5 (TM2H, nonsense; TM4, missense); a deletion in exon 5 (TM4); and an insertion in exon 7 (TM3). Although p53 protein was overexpressed in TM9 tumors, it was shown to be wild-type both by immunoprecipitation and direct sequencing of the entire coding region of the cDNA. TM4 cells were homogeneous with respect to mutant p53 genotype and uniformly expressed p53 by immunohistochemical staining in vitro, but transplantation of TM4 cells to fat pads of BALB/c hosts resulted in HAN outgrowths in situ in which < 50% of the cells expressed the mutant p53 at detectable levels. In summary, mutation of the p53 gene and overexpression of p53 protein can occur in preneoplastic mammary epithelial cells, and those mutations are maintained in tumors that arise from the HAN. Conversely, expression of mutant p53 was decreased when cells were grown in situ, implicating the presence of cellular factors that can suppress p53 expression in vivo. These observations demonstrate that the p53 pathway may be a common target for mutation in murine mammary tumorigenesis.(ABSTRACT TRUNCATED AT 400 WORDS)
乳腺的癌前病变代表了一群进展为肿瘤风险增加的细胞。由于p53是人类乳腺癌中最常发生突变的基因,我们试图确定p53突变是存在于癌前病变中还是在进展为明显肿瘤的过程中获得的。在小鼠乳腺中,增生性肺泡结节(HAN)是最常见的癌前病变。对可移植的小鼠HAN衍生瘤和肿瘤的TM系列进行分析,使得能够在乳腺肿瘤发生的不同阶段确定p53的状态。在所检测的所有5个HAN衍生瘤系中均观察到p53基因或p53蛋白表达模式的改变。通过免疫组织化学测定,在5个TM HAN衍生瘤系中的3个中检测到p53蛋白表达改变。在TM3和TM4 HAN衍生瘤中,仅在一部分细胞(10 - 50%)中检测到核p53的过表达,而在由TM4 HAN衍生瘤产生的肿瘤中,过表达p53蛋白的细胞比例接近100%。尽管TM3 HAN衍生瘤中p53过表达,但该系未发生肿瘤。TM9衍生瘤系通过免疫组织化学表现出不同的p53表达模式:p53蛋白在HAN衍生瘤中几乎所有细胞的细胞质中过表达,但定位于TM9肿瘤细胞的细胞核中。对肿瘤和细胞系的p53转录本进行直接测序揭示了各种基因变化:外显子4和5中的点突变(TM2H,无义突变;TM4,错义突变);外显子5中的缺失(TM4);以及外显子7中的插入(TM3)。尽管p53蛋白在TM9肿瘤中过表达,但通过免疫沉淀和cDNA整个编码区的直接测序显示其为野生型。TM4细胞在突变型p53基因型方面是同质的,并且在体外通过免疫组织化学染色均匀表达p53,但将TM4细胞移植到BALB/c宿主的脂肪垫中导致原位HAN衍生瘤,其中<50%的细胞以可检测水平表达突变型p53。总之,p53基因的突变和p53蛋白的过表达可发生在乳腺上皮癌前细胞中,并且这些突变在由HAN产生的肿瘤中得以维持。相反,当细胞原位生长时,突变型p53的表达降低,这意味着体内存在可抑制p53表达的细胞因子。这些观察结果表明,p53途径可能是小鼠乳腺肿瘤发生中常见的突变靶点。(摘要截断于400字)
