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对来自转移性和非转移性小鼠乳腺肿瘤的肿瘤相关巨噬细胞上的亮氨酸氨肽酶和酸性磷酸酶进行荧光激活细胞分选定量分析。

FACS quantitation of leucine aminopeptidase and acid phosphatase on tumor-associated macrophages from metastatic and nonmetastatic mouse mammary tumors.

作者信息

Mahoney K H, Miller B E, Heppner G H

出版信息

J Leukoc Biol. 1985 Nov;38(5):573-85. doi: 10.1002/jlb.38.5.573.

Abstract

Macrophages were isolated by adherence from tumors produced by a number of murine mammary carcinoma lines and were examined by fluorescence-activated cell sorting for quantitation of leucine aminopeptidase and acid phosphatase. The tumors included three lines, 66, 67, and 168, which were originally derived from a single, spontaneously arising tumor in a BALB/cfC3H mouse and two other lines, D2A1 and D2F2, which were derived from a single tumor arising from the transplantable hyperplastic alveolar nodule line, D2. These five lines differ from one another in a number of characteristics, including the ability to metastasize spontaneously to the lung from subcutaneous implants and to form experimental metastases in lungs following intravenous injection. Line 67 is nonmetastatic under both circumstances, whereas lines 66, D2A1, and D2F2 are metastatic under the same conditions. Intermediate to these is line 168, which is nonmetastatic from the subcutaneous site but capable of colonizing the lung with an efficiency similar to 66 when injected IV. Tumor-associated macrophages (TAM) from lines 66, D2A1, and D2F2 contained the greatest amounts of leucine aminopeptidase (LAP) and those from line 67 the least, with TAM from 168 being intermediate. Conversely, the TAM from line 67 had the greatest amounts of acid phosphatase (APTase) and those from line 168 the least. In addition to differences among tumors in enzyme levels of the adherent TAM, the precentages of TAM that were adherent were also different among the tumors. Only 12% of TAM from line 67 were recovered in the adherent fraction as opposed to 35-38% of TAM from lines 66 and 168. These results confirm and extend our previous findings that TAM from metastatic tumors have increased levels of LAP compared to TAM from nonmetastatic tumors. They also demonstrate noncoordinate expression of LAP and APTase in TAM, and illustrate how a population of TAM can be homogeneous for one enzyme and heterogeneous for another. Furthermore, the difference in the percentage of macrophages that are adherent between metastatic and nonmetastatic tumors is another indication both of the heterogeneous nature of TAM and of the role of a tumor in determining the type of host infiltrate with which it is associated.

摘要

通过贴壁法从多种小鼠乳腺癌细胞系产生的肿瘤中分离出巨噬细胞,并通过荧光激活细胞分选技术检测亮氨酸氨基肽酶和酸性磷酸酶的含量。这些肿瘤包括三个细胞系,66、67和168,它们最初源自一只BALB/cfC3H小鼠自发产生的单个肿瘤,另外两个细胞系,D2A1和D2F2,源自可移植增生性肺泡结节细胞系D2产生的单个肿瘤。这五个细胞系在许多特征上彼此不同,包括从皮下植入物自发转移至肺部以及静脉注射后在肺部形成实验性转移的能力。在这两种情况下,67细胞系都不具有转移性,而66、D2A1和D2F2细胞系在相同条件下具有转移性。介于两者之间的是168细胞系,它从皮下部位不具有转移性,但静脉注射时能够以与66细胞系相似的效率在肺部定植。66、D2A1和D2F2细胞系的肿瘤相关巨噬细胞(TAM)中亮氨酸氨基肽酶(LAP)含量最高,67细胞系的TAM中含量最低,168细胞系的TAM含量居中。相反,67细胞系的TAM中酸性磷酸酶(APTase)含量最高,168细胞系的TAM中含量最低。除了贴壁TAM的酶水平在肿瘤之间存在差异外,贴壁TAM的百分比在肿瘤之间也有所不同。67细胞系的TAM中只有12%在贴壁部分中回收,而66和168细胞系的TAM中这一比例为35 - 38%。这些结果证实并扩展了我们之前的发现,即与非转移性肿瘤的TAM相比,转移性肿瘤的TAM中LAP水平升高。它们还证明了TAM中LAP和APTase的非协同表达,并说明了一群TAM如何在一种酶上是同质的而在另一种酶上是异质的。此外,转移性和非转移性肿瘤之间贴壁巨噬细胞百分比的差异,既表明了TAM的异质性,也表明了肿瘤在决定与其相关的宿主浸润类型中的作用。

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