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女性/48岁 阴道肿块 [IHC标记2010-6-30]

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楼主 发表于 2010-05-13 18:51|举报|关注(0)
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简要病史:  阴道肿块10年,无明显症状,近期内增大。
肉眼检查:  肿块1.8x1.5x1.4cm, 边界清楚,无明显包膜。
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2 楼    发表于2010-07-08 01:04:00举报|引用
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以下是引用xhyong在2010-7-7 5:56:00的发言:

 可以向神经束膜瘤考虑。神经束膜瘤EMA CD34皆可阳性

Cytomorphology and stains do not support
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3 楼    发表于2010-07-07 08:33:00举报|引用
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非常好的诊断意见,如何与上皮样平滑肌瘤鉴别?

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4 楼    发表于2010-07-07 05:56:00举报|引用
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 可以向神经束膜瘤考虑。神经束膜瘤EMA CD34皆可阳性
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5 楼    发表于2010-07-03 20:03:00举报|引用
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谢谢Dr. Zhao! 本病例镜下的边界清楚,但是无完整的纤维包膜。

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6 楼    发表于2010-07-03 15:55:00举报|引用
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 Vaginal tumor, 1.8 cm, 边界清楚.

Microscopically the spindle shaped tumor cells show no atypica, no mitosis, with focal increase of cellularity.

Stains: Desmin, SMA positive, HMB45, melan A, s100 negative. CD34, 56, 57 stains are no specific.

I favor it is a leiomyoma-.平滑肌瘤

In the comment, I may mention that the tumor show focally increased cellularity, focally with epitheliod change. Vagina leomyoma is rare. Most likely the tumor will have a benign behavor . Close clinical follow-up is suggested.

Just for reference.

Dr. Jin: How about the tumor edge microscopically?

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7 楼    发表于2010-07-03 15:42:00举报|引用
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 Interesting case. Thank Dr. Jin for sharing. Notice a lot of good dicusion already and the papers djdnx provided. Thanks

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8 楼    发表于2010-07-01 21:26:00举报|引用
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 学习
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9 楼    发表于2010-07-01 18:45:00举报|引用
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感谢Dr.djdnx提供的诊断思路和文献!我将进一步IHC标记 CD117、Dog-1、 nestin、 CD10等抗体。也请网友建议标记抗体,谢谢!

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10 楼    发表于2010-07-01 16:32:00举报|引用
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本帖最后由 于 2010-07-01 17:24:00 编辑

学习中,现在的结果是免疫组化和形态学更倾向于上皮样平滑肌肿瘤。

浅薄的认识:HMB-45的结果对PEComa的诊断有抵触,作为一种通过形态学和免疫表型同时定义的肿瘤,本例可能不能诊断。

问题;1、本例中肿瘤细胞CD56和CD57的表达的意义是什么?

     2、第二篇文献,提示了CD56在胃肠间质瘤,平滑肌肿瘤,神经源性肿瘤的表达谱,不知本例中的CD56阳性的鉴别诊断意义?

     3、本例是否可以完全除外宫颈的胃肠道外间质瘤的可能?

     4、随访对于本例的认识有作用!

    

 

 

 

    

 

附关于PEComa的文献,和大家分享,鉴别诊断和讨论 

Malignant perivascular epithelioid cell tumor (PEComa) of the uterus with late renal and pulmonary metastases: a case report with review of the literature

Henry B Armah and Anil V Parwani

Department of Pathology, University of Pittsburgh Medical Center, Pittsburgh, PA, USA

author email corresponding author email

Diagnostic Pathology 2007, 2:45doi:10.1186/1746-1596-2-45

The electronic version of this article is the complete one and can be found online at: http://www.diagnosticpathology.org/content/2/1/45

Received:

27 September 2007

Accepted:

3 December 2007

Published:

3 December 2007

© 2007 Armah and Parwani; licensee BioMed Central Ltd.
This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

 

Abstract

Background

Perivascular epithelioid cell tumor (PEComa), other than angiomyolipoma (AML), clear cell sugar tumor (CCST), and lymphangioleiomyomatosis (LAM), is a very rare mesenchymal tumor with an unpredictable natural history. The uterus is the most prevalent reported site of involvement of PEComa-not otherwise specified (PEComa-NOS). To the best of our knowledge, about 100 PEComa-NOS have been reported in the English Language medical literature, of which 38 were uterine PEComa-NOS. These reported cases of uterine PEComa-NOS have usually shown clinically benign behavior, but 13 tumors, three of them associated with tuberous sclerosis complex (TSC), exhibited local aggressive behavior and four of them showed distant metastases.

Case presentation

We report the case of a 59-year-old woman, who presented with renal and pulmonary lesions seven years after the initial diagnosis of uterine leiomyosarcoma. Left nephrectomy and right middle lobe wedge resection were performed. Histological and immunohistochemical analysis of the renal and pulmonary lesions, in addition to retrospective re-evaluation of the previous uterine tumor, led to the final diagnosis of malignant uterine PEComa with late renal and pulmonary metastases. All three lesions had the typical histological appearance of PEComa-NOS showing a biphasic growth pattern with continuous transition between spindle cells and epithelioid cells, often arranged around vascular spaces. Immunohistochemically, the tumor cells of both phenotypes in all three lesions stained for melanocytic (HMB-45 and Melan-A/MART-1) and myoid (desmin, smooth muscle actin, and muscle-specific actin/all muscle actin/HHF-35) markers.

Conclusion

The findings indicate that despite the small number of reported cases, PEComas-NOS should be considered tumors of uncertain malignant potential, and metastases to other organs might become evident even several years after the primary diagnosis.

 

Background

The World Health Organization defines perivascular epithelioid cell tumors (PEComas) as "mesenchymal tumors composed of histologically and immunohistochemically distinctive perivascular epithelioid cells (PECs)" [1]. In 1991, Pea and colleagues [2] first noted this unusual cell in both angiomyolipoma (AML) and clear cell sugar tumor (CCST) of the lung. One year later, Bonetti and colleagues [3] proposed a cellular link between AML, CCST, and lymphangioleiomyomatosis (LAM), their association with tuberous sclerosis complex (TSC), and advanced the concept of a family of neoplasms composed of this distinctive cell which was "immunoreactive with melanocytic markers, and exhibit an epithelioid appearance, a clear-acidophilic cytoplasm, and a perivascular distribution". In 1996, Zamboni et al [4] reported the first case of pancreatic CCST and suggested the name PEComa for these neoplasms composed of a pure proliferation of PECs. There is no known normal cellular counterpart to this PEC, and a precursor lesion for PEComas has not been described [1]. Subsequently, the PEComa family of tumors has grown to include AML, CCST, LAM, and a number of rare unusual visceral, intraabdominal, soft tissue and bone tumors, which have been described under a variety of names, including "clear cell myomelanocytic tumor (CCMMT) of the falciform ligament/ligamentum teres", "abdominopelvic sarcoma of perivascular epithelioid cells", and "primary extrapulmonary clear cell sugar tumor", among others. This latter group of rare, morphologically and immunophenotypically similar tumors arising at a variety of visceral (commonly gastrointestinal, gynecological and genitourinary) and soft tissue (commonly retroperitoneal, abdominopelvic and cutaneous) sites have been collectively termed non-AML, non-LAM, non-CCST PEComas; or PEComas other than AML, LAM or CCST; or PEComas-not otherwise specified (PEComas-NOS) [1]. Generally, CCMMT is now not considered a distinct entity, but rather fall within the morphological spectrum of PEComas-NOS [1].

To the best of our knowledge, about 100 PEComas-NOS have been reported in the English Language medical literature, of which 38 were uterine PEComas-NOS [1,5-17]. These 38 reported cases of uterine PEComas-NOS have usually shown clinically benign behavior, but thirteen tumors exhibited locally aggressive behavior [5-9]. Three of these thirteen locally aggressive uterine PEComa-NOS were associated with TSC [5,6], whilst four of them showed distant metastases to liver, lungs, intestines, bone and lymph nodes up to seven years after resection of the uterine tumors [5,7,9]. Although there is a strong association between TSC, AML, LAM and CCST; this association is much less clear for the rarer PEComas-NOS [1]. Since relatively few cases of malignant PEComa have been reported and the duration of follow-up relatively short in the reported cases of PEComa, firm criteria for malignancy have yet to be established. However, a recent review report suggested criteria for malignancy including a size of >8.0 cm, mitotic count of >1 per 50 high-power fields (HPFs) and necrosis; and these three criteria helped to stratify PEComas into benign, uncertain malignant potential, and malignant [8]. Unfortunately, until more cases of this rare tumor are evaluated in a systematic fashion, firm criteria for malignancy remain uncertain. We report herein the case of a 59-year-old woman who presented with renal and pulmonary lesions seven years after the initial diagnosis of uterine leiomyosarcoma, but histological and immunohistochemical analysis of the renal, pulmonary and previous uterine lesions led to the final diagnosis of malignant uterine PEComa-NOS with late renal and pulmonary metastases.

 

Case presentation

A 59-year-old woman with a past medical history of hysterectomy and bilateral salpingo-ophrectomy for uterine leiomyosarcoma (American Joint Commission on Cancer Staging; AJCC T1c N0 M0; diagnosed at an outside institution) seven years prior presented to our institution for her regular periodic computed tomography (CT) scans of the abdomen, chest and pelvis at 6-month intervals as tumor follow-up investigations. These CT scans revealed several coalescing rim-enhancing nodules (altogether measuring 6.0 cm) in the upper and middle poles of her left kidney and a solitary rim-enhancing nodule (measuring 1.5 cm) in her right middle lobe of lung, which were absent on her previous CT scans six months earlier. The clinical impression was metastasis from her previous uterine leiomyosarcoma. No additional nodules were identified in the brain, gastrointestinal (GI) tract, liver, spleen, pancreas, bladder and bones on subsequent staging magnetic resonance imaging (MRI) of the brain, abdomen, chest and pelvis, and positron emission tomography (PET) scan. The patient did not have any stigmata or family history of TSC, and had no history of melanoma. General physical examination was unremarkable. Her hemogram, urine and blood biochemical analyses were within normal ranges.

A left radical nephrectomy and video-assisted thoracoscopic surgical wedge resection of the right middle lobe solitary nodule were performed. Grossly, her resected left kidney revealed a sharply demarcated and lobulated firm gray-tan nodular tumor (7.5 × 6.2 × 5.4 cm) occupying the upper and middle poles, and showed focally hemorrhagic areas on cut surface (Figure 1A). The interface between tumor and uninvolved kidney was sharp (Figure 1A). A 3.0 cm tan tumor thrombus protruded from the renal vein resection margin, whilst the renal artery and ureter resection margins were grossly free of tumor. The tumor grossly infiltrated into the renal sinus and extended broadly to, but not through, both the anterior and posterior renal capsules. Gross infiltration of tumor into the perinephric adipose tissue was absent. Her wedge-resected right middle lobe of lung revealed a sharply demarcated firm gray-tan nodule (2.3 × 2.2 × 2.0 cm) with focally hemorrhagic overlying pleura. The cut surface of the tumor was focally hemorrhagic. The tumor extends to, but not through the overlying pleura, and was at least 0.5 cm from the nearest stapled resection margin.

Figure 1. (A) Sharply demarcated gray-tan nodular tumor occupying the upper and middle poles with focally hemorrhagic areas on cut surface (Gross). (B) Biphasic renal tumor composed mainly of medium to large epithelioid cells and focal areas of spindle cells around numerous small blood vessels (H&E, Original magnification ×100). (C) Perivascular epithelioid cells arranged in solid nests or cords with well-defined cytoplasmic borders and abundant cytoplasm that varied from eosinophilic and granular to clear (H&E, Original magnification ×400). (D) Moderate-to-severe nuclei pleomorphism and hyperchromatism with bizarre multinucleated giant cells and mitoses (H&E, Original magnification ×400).

Histologically, the renal tumor was biphasic and composed mainly of medium to large epithelioid cells and focal areas of spindle/elongated cells around numerous small blood vessels (Figures 1B & 1C). The medium to large epithelioid neoplastic cells were arranged in solid nests or cords, and had well-defined cytoplasmic borders with abundant cytoplasm that varied from eosinophilic and granular to clear (Figure 1C). The nuclei of the epithelioid cells were mainly round, centrally located, and vesicular, with moderate-to-severe pleomorphism and hyperchromatism (Figures 1C &1D). Extensive cellular atypia, including bizarre multinucleated giant cells with large nuclei and nucleoli, was present (Figure 1D). Conspicuous nucleoli and mitoses were frequently present (Figure 1D). Mitotic count for the renal tumor was high (60 per 50 HPFs). There was microscopic evidence of tumor invasion of the renal sinus and the renal vein, and extensive neoplastic cell invasion of smaller veins. The adrenal gland was unremarkable and was not invaded by tumor, and the non-neoplastic kidney revealed mild nephrosclerosis.

Microscopic examination of the pulmonary tumor (not shown) exhibited the same morphological features as the renal tumor described above (Figures 1B–1D). The interface between tumor and uninvolved lung was sharp, and several foci of hemorrhage and necrosis were present. Mitotic count for the pulmonary tumor was high (45 per 50 HPFs). The non-neoplastic lung tissue was unremarkable (not shown). Based on her history of status post hysterectomy for uterine leiomyosarcoma (diagnosed at an outside institution) seven years prior and the biphasic histologic appearance of spindle and epithelioid cells (with clear cell areas) with prominent perivascular distribution of neoplastic cells in both the renal and pulmonary tumors, a diagnosis of malignant uterine PEComa with renal and pulmonary metastases was considered. The pathology report, original hematoxylin-eosin (H&E) slides, and formalin-fixed paraffin embedded blocks of the prior uterine tumor were requested from the outside institution. The original H&E slides and new H&E slides re-cut from the paraffin blocks were evaluated, and sections from all three lesions (uterine, renal and pulmonary) were concurrently subjected to immunohistochemical analysis. The pathology report from the outside institution indicated that the prior uterine tumor diagnosed as uterine leiomyosarcoma measured 6.0 cm in its greatest dimension, with a pathologic TMN staging of pT1c N0 M0. Microscopic examination of the previous uterine tumor (not shown) exhibited the same morphological features as both the pulmonary (not shown) and renal (Figures 1B–1D) tumors described above.

Immunohistochemically, both the epithelioid and spindle neoplastic cells of the renal tumor were strong and diffusely (>80% of the neoplastic cells) positive for desmin (cytoplasmic and membranous) {Ventana, Tucson, Ariz} [Figure 2A], HMB-45 (cytoplasmic) {Ventana} [Figure 2B], Melan-A/MART-1 (cytoplasmic) {BioCare Medical, Walnut Creek, CA}, smooth muscle actin (cytoplasmic and membranous) {Dako, Carpinteria, CA}, muscle-specific actin/all muscle actin/HHF-35 (cytoplasmic and membranous) {Dako} [not shown]. The estrogen receptor (ER) {Ventana} [Figure 2C] and progesterone receptor (PR) {Ventana} [Figure 2D] immunostains showed strong nuclear reactivity in 60–80% and 30–50% of tumor cells, respectively. The renal tumor cells were strong and diffusely (>80% of the neoplastic cells) positive for BCL-2 (cytoplasmic and membranous) {Ventana} [Figure 3A], CD99 (membranous) {Ventana} [Figure 3B], and cyclin D1 (nuclear) {Ventana} [not shown]. A proliferative index of 70% was noted with Ki67 immunostaining (nuclear) {Ventana} [Figure 3C]. The tumor cells showed focal (<20% of the neoplastic cells), but strong, immunoreactivity for c-kit/CD117 (membranous) {Ventana}, vimentin (cytoplasmic and membranous) {Ventana}, epithelial membrane antigen (EMA) {cytoplasmic and membranous} [Ventana], and CD10 (membranous) {Ventana} [not shown]. The renal neoplastic cells failed to stain with antibodies against renal cell carcinoma marker (RCC) {Ventana} [Figure 3D], S-100 protein (Ventana), chromogranin (Ventana), cytokeratins (AE1/AE3, 8/18, 7/20) {Ventana}, CD34 (Ventana), and myogenin (Ventana) {not shown}. The immunoprofile of the pulmonary (not shown) and uterine (not shown) tumors were identical to that of the renal tumor described above (Figures 2A–2D & Figures 3A–3D). For all the three tumors in general, staining for the melanocytic markers (HMB-45 and Melan-A) were more intense in the epithelioid cells compared to the spindle cells. Staining for the myoid markers (desmin, smooth muscle actin, and muscle-specific actin) were variable in the cytoplasm and more prominent adjacent to the cytoplasmic membrane, and more intense in the spindle cells compared to the epithelioid cells. Positive controls were used for all markers as follows: HMB-45 and Melan-A – melanoma; RCC – renal cell carcinoma; S100 – schwannoma; desmin, smooth muscle actin, muscle-specific actin, and myogenin – GI smooth muscle; CD117 – GI mast cells and Cajal cells; cytokeratins – GI epithelial tissue; vimentin – GI mesenchymal tissue; and CD34 – tonsillar endothelial tissue. Slides stained omitting the primary antibody were used as negative controls.

Figure 2. Immunohistochemical staining of renal tumor. (A) Both epithelioid and spindle cells were strong and diffusely positive for desmin (Immunoperoxidase, Original magnification ×200). (B) Both epithelioid and spindle cells were strong and diffusely positive for HMB-45 (Immunoperoxidase, Original magnification ×200). (C) Estrogen receptor (ER) immunostaining showed strong and diffuse nuclear reactivity in tumor cells (Immunoperoxidase, Original magnification ×200). (D) Progesterone receptor (PR) immunostaining showed strong and moderate nuclear reactivity in tumor cells (Immunoperoxidase, Original magnification ×200).

Figure 3. Immunohistochemical staining of renal tumor. (A) Tumor cells showed strong and diffusely reactivity for BCL-2 (Immunoperoxidase, Original magnification ×200). (B) Tumor cells showed strong and diffusely reactivity for CD99 (Immunoperoxidase, Original magnification ×200). (C) Ki67 immunostaining showed a proliferative index of 70% (Immunoperoxidase, Original magnification ×200). (D) Tumor cells showed negative reactivity for renal cell carcinoma marker (RCC) (Immunoperoxidase, Original magnification ×200).

On the basis of the above histopathological and immunohistochemical features, a definitive diagnosis of malignant uterine PEComa with late renal and pulmonary metastases was rendered. The patient elected not to have any adjuvant chemotherapy or radiotherapy. Five follow-up CT scans of the brain, abdomen, chest and pelvis, and PET scans performed at 3-month intervals after surgery revealed no nodules. She is alive with no evidence of local recurrence or distant metastasis after 15 months of follow-up, and scheduled to have regular periodic CT scans of the abdomen, chest and pelvis at 3-month intervals as her tumor follow-up plan.

 

Discussion

In this report, we describe a case of unusual epithelioid tumors in the kidney and the lung seven years after the initial diagnosis of uterine leiomyosarcoma, with pathological and immunohistochemical features entirely compatible with those of a PEComa. PEComas are characterized by epithelioid to spindle cells with eosinophilic to clear cytoplasm, an intimate relationship with blood vessels, and demonstrate positive immunostaining for markers of both melanocytic (HMB45, Melan-A, tyrosinase, microphthalmia transcription factor) and myoid (desmin, smooth muscle actin, muscle-specific actin, caldesmon, calponin) differentiation [1]. PEComas-NOS have now been reported in almost every body site and the growing list of reported sites include gynecological, genitourinary, gastrointestinal, extremities and the skin, as well as single reports in the heart, breast, oral cavity, orbit, and skull base [1,5-17]. The uterus is the most prevalent reported site of involvement of PEComa-NOS (accounting for 38 out of about 100 reported cases). The other common sites are the gastrointestinal tract, genitourinary tract and retroperitoneum, whilst rare sites include somatic soft tissue, skin and bone. Almost all the reported non-uterine PEComas-NOS have been in women [1,5-17]. The vast majority of PEComas-NOS have been described in females (as in the case herein presented) [1,5-17], and therefore hormones may play a role in their pathogenesis and/or phenotypic cellular manifestations. Estrogen receptor (ER) and progesterone receptor (PR) expression, that have been reported primarily in the spindle cell component of PEComas [5,10], may play a role in the development of this morphologic pattern. The case herein presented showed moderate-to-strong positive nuclear staining for both ER and PR in both the spindle and epithelioid cell components of all three lesions (uterine, renal and pulmonary), although the ER staining was always more intense than PR staining.

PEComas are of interest primarily because of their immunoreactivity with melanocytic and myoid markers. They are also almost always negative for S-100 protein and cytokeratins. Folpe and colleagues [8] recently reviewed all reported cases of PEComa up to 2005 (61 cases). In their review, 100% were HMB-45 positive, 59% were smooth muscle actin positive, 41% were Melan-A positive, 33% were CD117 positive, 31% were desmin positive, 11% were S-100 positive, and 0% was cytokeratin positive. Therefore, nearly all PEComas are immunoreactive for HMB-45 and/or Melan-A, and many are positive for smooth muscle actin, whereas desmin staining appears to be somewhat less common. Elongated spindle cells in PEComas are characterized by prominent smooth muscle-specific filaments, while the epithelioid component does not usually contain high numbers of such filaments [8]. The case herein presented showed strong and diffuse staining for both HMB-45 and MelanA in both the spindle and epithelioid cell components of all three lesions (uterine, renal and pulmonary), with more intense staining in the epithelioid cells compared to the spindle cells. In the present case, staining for muscle-specific actin, smooth muscle actin, and desmin was more evident in the area adjacent to the cytoplasmic membrane, with more intense staining in the spindle cells compared to the epithelioid cells.

Not unexpectedly, the uterine tumor of the case herein presented was initially misdiagnosed as a uterine leiomyosarcoma at an outside institution seven years prior. Myomelanocytic marker expression was found to be prominent in both components of all the three lesions in the case herein presented. Controversy exists regarding the minimum criteria for the diagnosis of malignant PEComa [18,19]. In studies of uterine tumors demonstrating epithelioid morphology, clear cell areas and HMB-45 positivity, these authors [18,19] argued that these lesions represented epithelioid smooth muscle tumors with focal melanocytic differentiation and not PEComas. This view was based largely on the fact that the tumors looked like classic leiomyosarcomas with spindled and epithelioid areas, and stained with desmin. Nevertheless, these authors [18,19] still advocated performing immunohistochemistry for HMB-45 in all uterine epithelioid smooth muscle tumors, in order to identify patients who should be investigated for TSC. It is also noteworthy that only focal HMB-45 staining was seen in their cases, unlike the diffuse expression in the case herein presented and nearly all the reported cases of uterine PEComa [1,5-11]. Additionally, 31% of PEComas showed at least focal desmin staining in a recent review of all reported cases up to 2005 (61 cases) [8], and therefore desmin staining of uterine epithelioid tumors with clear cell areas and HMB-45 positivity does not exclude the diagnosis of PEComa. We are therefore of the view that tumors with diffuse myomelanocytic differentiation should be regarded as being related to the PEComa family irrespective of site of origin or desmin positivity, and that it is the characteristic morphology and immunophenotype that warrants separating these tumors from classic leiomyosarcoma that exhibit only muscle differentiation. However the clinicopathological significance of HMB-45 positivity in uterine epithelioid smooth muscle tumors is not known.

In addition to epithelioid smooth muscle tumors (epithelioid leiomyosarcoma and epithelioid leiomyoma), the other important differential diagnosis of PEComa include malignant melanoma, clear cell sarcoma of tendon and aponeuroeses (melanoma of the soft parts), alveolar soft part sarcoma, endometrial stromal sarcoma with clear cell features, uterine tumor resembling sex cord tumor, carcinoma (especially renal cell and adrenocortical carcinoma), paraganglioma, angiomyolipoma, and any other tumor with focal or prominent clear cell change. Malignant melanoma and clear cell sarcoma of tendon and aponeuroeses can be differentiated from PEComas based on S-100 positivity; however, up to 11% of PEComas express S-100 as well [8]. The additional important features for the diagnosis of PEComa in this context include negative history for melanoma, visceral location of tumor, perivascular accentuation of tumor cells, immunoreactivity for myoid markers (smooth muscle actin, muscle-specific actin, and desmin), and absence of the t(12:22) translocation. Although S-100 negative melanomas have rarely been described, tumors with S-100 negativity, strong and diffuse melanocytic marker positivity, and actin immunoreactivity should be designated as PEComas based on morphology and immunophenotype. Pitfalls in the diagnosis of PEComas include aberrant staining of cells with melanocytic markers. However, diffuse and multiple melanocytic marker expression is highly reliable for melanocytic differentiation. Focal or weak positivity can be disregarded, however, and do not warrant the diagnosis of PEComa. The case herein presented was strong and diffusely positive with at least two melanocytic markers (HMB45 and Melan-A), which is not a finding in other sarcomas. Angiomyolipoma can be ruled out because the present case lacked lipomatous elements and showed a biphasic cellular population. However, PEComa and monophasic epithelioid angiomyolipoma are probably very closely related, if not the same entity. Endometrial stromal sarcoma and uterine tumor resembling sex cord tumor can be ruled out because of the presence of prominent perivascular accentuation of tumor cells and diffuse, rather than focal, positive staining of HMB-45 in PEComa. PEComa can be distinguished from paraganglioma in that the former is negative for chromogranin A, synaptophysin, and S-100 protein, and the latter shows more organoid growth. The expression of melanocytic markers (HMB-45 and MART-1/Melan-A) and the lack of immunoreactivity for cytokeratins and RCC marker argue against the diagnosis of carcinoma.

Clinically, most PEComas follow a benign course [1]. Malignant PEComas-NOS are being increasingly reported, several originating in the uterus and others arising in the jejunum, ileum, prostate, pelvis, skull base, broad ligament and somatic soft tissue [1,5-17]. Since relatively few malignant PEComas have been reported, firm criteria for malignancy have yet to be established. However, Folpe and colleagues [8] recently suggested criteria for malignancy including a size of >8.0 cm, mitotic count of >1 per 50 high power fields (HPFs) and necrosis, with benign, uncertain malignant potential and malignant categories based on the presence of none, 1 or ≥ 2 of these three criteria, respectively. Infiltrative growth or edges, marked hypercellularity and marked nuclear pleomorphism/atypia may be secondary features suggesting aggressive behaviour or malignancy [1,8,11]. A Ki-67 labeling index of 5% of neoplastic cells has been observed in a uterine PEComa that have behaved aggressively [7]. In the case herein presented, the size of the primary uterine tumor seven years prior was <8 cm, mitotic count was >1 per 50 HPFs and necrosis was absent. Retrospectively, this uterine tumor would be categorized as of uncertain malignant potential according to the above suggested criteria. Additionally, the uterine tumor showed all the three secondary features suggestive of aggressive behaviour or malignancy. Furthermore, the Ki-67 labeling index was greater than 5% in the uterine tumor (also in the renal and pulmonary metastases), and thus the uterine tumor was destined to behave aggressively, which it did seven years later. Dimmler and colleagues have also reported late pulmonary metastases occurring seven years after the diagnosis of a case of uterine PEComa [7]. Therefore, metastatic spread of PEComas may, in some cases, be a late complication, presenting after many years. This highlights both the need for criteria that more accurately predict the behavior of PEComas and the need for long-term follow-up of patients with PEComas, as widespread metastases may present as a late complication.

Optimal treatment for PEComas is not well established at this time. Currently, surgery is the mainstay of treatment for primary PEComa at presentation as well as for local recurrences and metastases, with the aim of obtaining clear resection margins. The role of adjuvant therapy remains unclear. Metastases have been successfully managed by resection alone [7]. Primary excision is usually curative, as most PEComas are benign. However, locally advanced or metastatic disease portends a poor prognosis and treatment strategies incorporating surgery, radiotherapy and chemotherapy have been reported [20]. Given the uncertainty of PEComa tumor biology, adjuvant therapies, including chemotherapy and immunotherapy, may be considered for patients with locally advanced or metastatic PEComa.

 

Conclusion

We have described a case of malignant PEComa-NOS of the uterus with late renal and pulmonary metastases seven years after hysterectomy. Malignant PEComa should be considered in the light microscopic differential diagnosis for all pleomorphic sarcomas. PEComas-NOS show a marked female predominance, are rare but anatomically ubiquitous mesenchymal tumors that are composed of nests and sheets of usually epithelioid but occasionally spindled cells with clear to granular eosinophilic cytoplasm and a focal association with vascular spaces. They usually show immunoreactivity for both melanocytic (HMB-45 and/or Melan-A/Mart-1) and myoid/muscle-specific (actin and/or desmin) markers, which are useful for confirming the diagnosis. The mainstay of treatment is wide excision. Though most PEComas are benign, a subset behaves in a malignant fashion; size >8 cm, high mitotic index, presence of necrosis, marked cytological atypia, and/or infiltrative growth pattern may be associated with malignant behavior. However, since relatively few malignant PEComas have been reported, firm criteria for malignancy have yet to be established and the identity of the normal PEC remains elusive. Further studies on additional cases with longer clinical follow-up would be necessary to accurately predict the biologic behavior of these distinctive tumors. Finally, because PEComas can behave in an aggressive manner, careful follow up is warranted.

    

 

 

 

文献二

 

J Clin Pathol doi:10.1136/jcp.2007.052696

Distribution of neural cell adhesion molecule (NCAM/CD56) in GISTs and their intra-abdominal mesenchymal mimics

1.     Abbas Agaimy (abbas.agaimy@klinikum-nuernberg.de)

+ Author Affiliations

1.     Institute of Pathology, Nuremberg Clinic Center, Germany

1.     Peter H. Wünsch (wuensch@klinikum-nuernberg.de)

+ Author Affiliations

1.     IInstitute of Pathology, Nuremberg Clinic Center, Germany

·         Published Online First 8 October 2007

Abstract

Background: To our knowledge, the distribution and reactivity pattern of neural cell adhesion molecule (NCAM/CD56) in GI stromal tumours (GIST) and their mesenchymal mimics have not been investigated in the KIT era. Methods: We analysed a total of 275 histologically and immunohistochemically well characterised primary and metastatic intra-abdominal mesenchymal lesions by conventional Immunohistochemistry, with emphasis on GIST and GI smooth muscle neoplasms. Results: CD56 expression was seen in 18/21 (86%), 4/5 (80%), 26/34 (76%), and 32/168 (19%) of primary GI leiomyomas, schwannomas, leiomyosarcomas, and GISTs, respectively. Reactivity in GISTs was mostly focal. Of 6% strongly staining GISTs, 71% were either malignant clinically or assigned a high risk prognostic group. CD56 expression in GISTs varied greatly with histologic type (seen in 50%, and 7% of epithelioid and spindled GISTs, respectively) and anatomic site (in 33%, 10%, 1%, and 0% of rectal, gastric, small intestinal and oesophageal GISTs, respectively). A variable, but inconsistent expression was seen in miscellaneous lesions including dedifferentiated liposarcoma, abdominopelvic PEComas, myo/fibroblastic sarcoma and "MFH". Mesenteric fibromatoses, angiosarcoma/Kaposi sarcoma, reactive tumefactive fibrogenic lesions and 12 of 13 primary anorectal and oesophageal melanomas were negative. Conclusion: Our results confirmed the ubiquity and non-specificity of CD56 as a neurogenic marker. Except for a subset of epithelioid gastric and high-grade rectal lesions, CD56 expression is rare in GISTs, contrasting with leiomyomatous and neurogenic neoplasms. CD56 plays a limited role in the differential diagnosis of GIST. Its potential role as a marker of adverse outcome in GISTs remains to be further investigated.

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11 楼    发表于2010-07-01 08:24:00举报|引用
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有意思!!

谢谢金老师的病例!

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12 楼    发表于2010-06-30 18:18:00举报|引用
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本帖最后由 于 2010-07-01 05:57:00 编辑

 

IHC标记:图1-3 CD34;图4-5 CD56;图6-7 CD57; 图 8-9 S-100; 图11-12 GFAP; 图13 Desmin; 图14 SMA; 图15 ER。

其他标记:AE1/AE3-、Cam5.2-、CD31-、p63-、Ki-67(5%)、WT-1 -、HMB-45 -、Melana -。

 

此病例形态和IHC标记都很特殊, 肿瘤细胞表达CD34、EMA、SMA/Desmin、CD56/CD57、ER;肿瘤边缘和肿瘤结节之间有神经纤维。

诊断为良性间叶性肿瘤、组织学类型比较难确定,请大家提供宝贵意见,谢谢!

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13 楼    发表于2010-06-14 22:46:00举报|引用
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 平滑肌肿瘤与PEComa鉴别。

不知标记如何。

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14 楼    发表于2010-06-14 19:55:00举报|引用
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 平滑肌瘤
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15 楼    发表于2010-06-14 19:54:00举报|引用
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 平滑肌瘤
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16 楼    发表于2010-06-13 18:22:00举报|引用
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 肿瘤体积小,生长过程近10年,细胞无显著异形,应该考虑良性可能大些,最多中间性。片中似乎没见腺样结构,不像上皮性的肿瘤。局部细胞疏松似有脂质样改变。
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17 楼    发表于2010-06-13 18:16:00举报|引用
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 不知道以前是否有过手术或产伤史,瘤细胞梭形,疏松,有大量胶元,其中有灶性炎症细胞,瘤细胞核相温和,无显著异形,考虑是否炎性肌纤维母细胞瘤。
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18 楼    发表于2010-06-13 17:51:00举报|引用
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 病变为双相性(上皮样+梭形),疏密不一。
上皮样区有些大空泡,不知是退变还是脂肪。
图16上皮细胞围绕一个小血管,但不呈放射状。
图12似乎有几个小腺腔。

大多数阴道恶性肿瘤(80%~99%)为转移性,通过直接扩散、淋巴和血行途径累犯阴道。它们最常发生于阴道上1/3的后壁。原发性阴道恶性肿瘤罕见,占所有妇产科癌症的1%~2%。这些原发性肿瘤中,约85%为鳞癌,其他为腺癌,以及罕见病变如透明细胞癌和肉瘤。
本例有十年病史,原发的可能性大。
考虑:
转移癌(透明细胞癌),不符合十年病史
上皮样血管平滑肌脂肪瘤(PEComa),但血管不明显
SFT,但胶原不明显
上皮样平滑肌瘤,但是有腺样结构。如果是假腺,尚可解释
其它软组织肿瘤
第一批免疫组化:CK,HMB45,SMA,CD34。
谢谢金老师!

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19 楼    发表于2010-06-13 17:24:00举报|引用
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以下是引用xljin8在2010-5-22 4:43:00的发言:

感谢您的宝贵建议。原始照片用Photoshop压缩后画面变小了, 我会努力解决这一问题。谢谢!

Photoshop处理过的图片,画质不会降低,图片一般会更大。

我一般用Photoshop仅用“图像-调整-自动对比度”处理图像,快捷键为“Alt+Ctl+Shift+L”。

然后选一块需要的画面“裁切”,快捷键为“Alt+I+P”。

再设定图像大小,快捷键为“Alt+I+I”,最少用1024X768。宽度与高度的比较是锁定的,一般只要设宽度就行了。我一般设1200或更大,这样点出的图像还能再放大。

另存为JPG格式。选最高品质,这样图像质量不会降低。

这时图像很大,不能上传。用其它小软件减肥。我用的是老版本ACDSee3.23,打开后另存为原文件名即可。至少能减肥2倍,而且图像质量不降低。此时适合上传。

如果熟悉快捷键,图像处理速度很快,整个过程大概30秒。

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20 楼    发表于2010-05-25 22:29:00举报|引用
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 低倍,考虑癌
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