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乳腺纤维腺瘤和一些叶状肿瘤的间质由CD34+成纤维细胞和因子XIIIa+树突状细胞组成。

Mammary fibroadenoma and some phyllodes tumour stroma are composed of CD34+ fibroblasts and factor XIIIa+ dendrophages.

作者信息

Silverman J S, Tamsen A

机构信息

Department of Pathology and Laboratory Medicine, Southampton Hospital, New York 11968, USA.

出版信息

Histopathology. 1996 Nov;29(5):411-9. doi: 10.1046/j.1365-2559.1996.d01-510.x.

Abstract

Fibroadenomas and mammary phyllodes tumour arise by proliferation of mammary stroma and epithelial elements. However, it is the stromal element that determines the biology of these biphasic tumours. Normal mammary stroma, like most collagenous connective tissue, contains resident populations of CD34+ dendritic interstitial cells and scattered factor XIIIa+ collagen-associated dendrophages. Actin+myofibroblasts are usually absent from mammary stroma in non-disease states. To determine whether CD34+ and factor XIIIa+ cells proliferate in fibroadenomas and phyllodes tumours, and to study myofibroblastic differentiation in these lesions, we examined 19 fibroadenomas in 14 patients along with five low grade and two high grade phyllodes tumours. We employed antibodies against the human progenitor cell antigen CD34, coagulation factor XIIIa and HHF-35 actin. In three fibroadenomas and two phyllodes tumours, we used Ki-67 antigen to study cell proliferation and oestrogen and progesterone receptors to study possible hormonal influence on stromal cells. In all fibroadenomas, CD34 strongly stained interlobular, pericanalicular and intracanalicular fibroblasts with collagenous and/or myxoid features. Four low grade phyllodes tumours also had CD34+ fibroblasts as did one high grade tumour. Actin reactivity varied and was most pronounced in six fibroadenomas resembling the so-called cellular variant, while seven regular fibroadenomas had no actin+stromal cells and six had only focal and weak actin+stromal cells. Factor XIIIa+ cells were prominently admixed in the stroma of all tumours studied comprising from 5% to 20% in fibroadenomas and, focally, up to 50% in phyllodes tumours. Oestrogen and progesterone receptors were expressed only in glandular elements. Ki-67 index in stromal cells was 1% to 3% in fibroadenoma, 10% to 20% in low grade, and 20% to 40% in high grade phyllodes tumour. We conclude that fibroadenomas and some phyllodes tumours are composed of CD34+ fibroblasts that show varying myxoid, collagenous or myofibroblastic differentiation. The fibroblasts are accompanied by a subset of dendritic histiocytes that express factor XIIIa. Fibroadenoma variants show prominent collagenous actin+myofibroblastic differentiation of CD34+ stromal cells, sometimes with a gradient of CD34 down-regulation. Fine-needle or limited stereotactic core biopsy of these biphasic tumours, if they yield only stromal cells, must be distinguished from other CD34+ stromal tumours. Increased factor XIIIa+ dendrophage populations were seen in phyllodes tumours, especially in two high grade tumours that had malignant fibrous histiocytoma-like features, suggesting clonal evolution toward the fibrohistiocytic final pathway. Further study of CD34 and factor XIIIa+ mammary stromal cells in larger numbers of phyllodes tumours might ascertain whether increasing factor XIIIa reactivity correlates with differentiation and increased tumour aggressiveness.

摘要

纤维腺瘤和乳腺叶状肿瘤由乳腺间质和上皮成分增殖形成。然而,决定这些双相性肿瘤生物学行为的是间质成分。正常乳腺间质,如同大多数胶原性结缔组织一样,含有CD34⁺树突状间质细胞和散在的因子ⅩⅢa⁺胶原相关树突状巨噬细胞。在非疾病状态下,乳腺间质中通常不存在肌动蛋白⁺肌成纤维细胞。为了确定CD34⁺和因子ⅩⅢa⁺细胞在纤维腺瘤和叶状肿瘤中是否增殖,并研究这些病变中的肌成纤维细胞分化情况,我们检查了14例患者的19个纤维腺瘤以及5个低级别和2个高级别叶状肿瘤。我们使用了针对人类祖细胞抗原CD34、凝血因子ⅩⅢa和HHF - 35肌动蛋白的抗体。在3个纤维腺瘤和2个叶状肿瘤中,我们使用Ki - 67抗原研究细胞增殖情况,并使用雌激素和孕激素受体研究激素对间质细胞可能产生的影响。在所有纤维腺瘤中,CD34强烈染色具有胶原性和/或黏液样特征的小叶间、腺管周围和腺管内成纤维细胞。4个低级别叶状肿瘤以及1个高级别肿瘤也有CD34⁺成纤维细胞。肌动蛋白反应性各不相同,在6个类似所谓细胞型的纤维腺瘤中最为明显,而7个普通纤维腺瘤没有肌动蛋白⁺间质细胞,6个仅有局灶性且弱阳性的肌动蛋白⁺间质细胞。因子ⅩⅢa⁺细胞显著混合存在于所有研究肿瘤的间质中,在纤维腺瘤中占5%至20%,在叶状肿瘤中局部可达50%。雌激素和孕激素受体仅在腺上皮成分中表达。纤维腺瘤中间质细胞的Ki - 67指数为1%至3%,低级别叶状肿瘤为10%至20%,高级别叶状肿瘤为20%至40%。我们得出结论,纤维腺瘤和一些叶状肿瘤由显示出不同黏液样、胶原样或肌成纤维细胞分化的CD34⁺成纤维细胞组成。这些成纤维细胞伴有表达因子ⅩⅢa的树突状组织细胞亚群。纤维腺瘤变体显示出CD34⁺间质细胞明显的胶原性肌动蛋白⁺肌成纤维细胞分化,有时伴有CD34下调梯度。对于这些双相性肿瘤,如果细针穿刺活检或有限的立体定向核心活检仅获取到间质细胞,则必须与其他CD34⁺间质肿瘤相鉴别。在叶状肿瘤中,尤其是在2个具有恶性纤维组织细胞瘤样特征的高级别肿瘤中,可见因子ⅩⅢa⁺树突状巨噬细胞数量增加,提示向纤维组织细胞最终途径的克隆性演变。对更多叶状肿瘤中CD34和因子ⅩⅢa⁺乳腺间质细胞的进一步研究可能会确定因子ⅩⅢa反应性增加是否与分化及肿瘤侵袭性增加相关。

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