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姓名：	×××	性别：	男	年龄：	70
标本名称：	腮腺肿物，肿瘤中央质地坚硬如骨，镜下中央区呈变性状，仅见粘液软骨样基质，无细胞，所传图片为肿瘤周边。
简要病史：
肉眼检查：

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本帖最后由于 2010-09-13 21:18:00 编辑

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: 嫁人就嫁灰太狼，学习要上华夏网。

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yixuerensheng 离线: 帖子：25; 粉蓝豆：92; 经验：68; 注册时间：2010-03-28; 加关注 | 发消息

1 楼发表于2010-10-09 23:04:00举报|引用
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癌

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wang4160 离线: 帖子：2256; 粉蓝豆：16; 经验：2617; 注册时间：2007-01-31; 加关注 | 发消息

2 楼发表于2010-10-09 08:49:00举报|引用
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太有意思了，真想看一看切片，了解一下全貌！

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wfbjwt 离线: 帖子：6628; 粉蓝豆：163; 经验：7418; 注册时间：2006-10-08; 加关注 | 发消息

3 楼发表于2010-10-08 18:36:00举报|引用
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谢谢明月老师提醒，不过我认为肿瘤部分确实绝大部分细胞阳性，与灶性分化不同，另外因图片不清，故上述图片中专门选择了一些做正常导管上皮对照。

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: 嫁人就嫁灰太狼，学习要上华夏网。

海上明月离线: 帖子：9476; 粉蓝豆：1172; 经验：10007; 注册时间：2009-08-29; 加关注 | 发消息

4 楼发表于2010-10-04 16:26:00举报|引用
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以下是引用海上明月在2010-10-4 15:59:00的发言：

以下是引用wfbjwt在2010-10-4 8:42:00的发言：

请教明月老师：导管癌是腺上皮起源，P63是否应阴性？我很羡慕大家找外文文献都这么容易。

唾腺导管癌表达P63阴性。但是，如果导管癌伴有鳞状分化的时候可灶性P63阳性。这与本例比较符合。

肿瘤中残留的良性病变或陷入的数量正常导管也可灶性表达P63阳性。

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: 王军臣

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5 楼发表于2010-10-04 15:59:00举报|引用
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以下是引用wfbjwt在2010-10-4 8:42:00的发言：

请教明月老师：导管癌是腺上皮起源，P63是否应阴性？我很羡慕大家找外文文献都这么容易。

唾腺导管癌表达P63阴性。但是，如果导管癌伴有鳞状分化的时候可灶性P63阳性。这与本例比较符合。

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: 王军臣

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6 楼发表于2010-10-04 12:52:00举报|引用
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根据形态结构，是不是本例考虑为导管癌更好些。

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: 王军臣

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7 楼发表于2010-10-04 09:34:00举报|引用
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Salivary duct carcinoma in the sinonasal tract.

Higo R, Takahashi T, Nakata H, Harada H, Sugasawa M.

Department of Otolaryngology, Head and Neck Surgery, Saitama medical university, Morohongo 38, Moroyama-cho, Iruma-gun, Saitama, Japan. rhigo-tky@umin.ac.jp

Abstract

Salivary duct carcinoma (SDC) is an uncommon malignant tumor, characterized by aggressive behavior and poor prognosis. SDC usually arises from ductal epithelium of the major salivary glands, and it is quite infrequent elsewhere. We present a rare case of a 73-year-old man with SDC, which is possibly originated from the paranasal sinuses or the lacrimal system. Microscopic evaluation revealed that the tumor cells, with pleomorphic nuclei and abundant eosinophilic cytoplasm, formed cell nests and duct-like structure. A cribriform growth pattern was also seen. Immunohistochemical staining was positive for cytokeratins (CAM 5.2 and 34betaE12), gross cystic disease fluid protein 15 (GCDFP-15), and androgen receptor protein, while p63 and involucrin were negative. The patient already had multiple metastasis of the tumor in the lung at diagnosis, and he could not undergo definitive surgical procedures, because of severe restrictive lung disease. Although SDC in the sinonasal tract is quite rare, SDC should be in the differential diagnosis in these regions, due to its aggressive behavior and poor prognosis.

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8 楼发表于2010-10-04 09:33:00举报|引用
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Salivary duct carcinoma cytologically diagnosed distinctly from salivary gland carcinomas with squamous differentiation.

Kawahara A, Harada H, Akiba J, Kage M.

Department of Pathology, Kurume University Hospital, Japan. akihiko4@med.kurume-u.ac.jp

Abstract

It has been difficult cytologically to distinguish salivary duct carcinoma (SDC) from high-grade carcinoma. We investigated the microscopic cytological findings, morphometric image analyses, and immunohistochemical features of SDC, focusing on how we achieved an accurate differential diagnosis distinguishing SDC from salivary gland carcinomas with squamous differentiation. Immunohistochemical staining was performed for androgen receptor (AR), gross cystic disease fluid protein-15 (GCDFP15), mammaglobin, human gastric mucin, MUC1, MUC2, p63, and cytokeratin high molecular weight. Of the 13 cases of SDC, 9 cases showed typical cytological findings of sheet clusters with polygonal granular cytoplasm with fine chromatin. The other 4 cases showed unusual cytological findings of a pseudo-papillary cluster or scattered cells only, and the tumor cells showed coarse chromatin. Morphometric image analysis showed that the nucleus area was statistically different between SDC and salivary gland carcinomas with squamous differentiation. AR-positive expression (P = 0.008), GCDFP15-positive expression (P = 0.005) and p63-negative expression (P = 0.001) were effective as SDC-specific markers in immunohistochemistry. An accurate cytological diagnosis of SDC can be determined by immunostaining with AR, GCDFP15, and p63, based on the nuclear findings.