Effect and mechanism of atropine and mepyramine on histamine-induced plasma leakage and serous cell secretion in the rat trachea

Chang, Jui-Hsin

14 July 2004

Many factors influence the inflammatory responses in rat trachea, including inflammatory mediators released from nerve fibers, histamine released by mast cells and endotoxin from the cell walls of bacteria. The inflammatory responses include plasma extravasation, subepithelial edema, and hypersecretion of secretory cells. But the mechanism of inflammation mediated by these factors was not completely understood. In the present study, a high dose of histamine was administered intravenously to induce the inflammation in rat airway. India ink was also injected as a tracer to label the leaky blood vessels in different time points. To investigate the serous cell secretion and subepithelial edema formation, the treacheal tissue was processed for histological study. Electron microcopy was carried out to investigate the ultrastructure of serous cells. To investigate the mechanism of histamine effect, the muscarinic receptor antagonist atropine (1 mg/ml/kg) or histamine H1 receptor antagonist mepyramine (10 mg/ml/kg) was injected 15 min before histamine injection. Five minutes after histamine, plasma leakage and serous cell secretion were extensive. The area density of India ink-labeled leaky vessels was 17.24 % ¡Ó 2.03 %. Saline, the vehicle of histamine, produced only a little extravasation. Mepyramine inhibited the histamine-induced plasma extravasation and serous cell degranulation significantly but atropine had no effect. The results suggest that histamine-induced serous cell degranulation is mainly through histamine H1 receptors but not through cholinergic muscarinic receptors in rat trachea.

trachea

histamine

plasma extravasation

inflammation

serous cell

IMP3 as a cytoplasmic biomarker for early serous tubal carcinogenesis

Wang, Yiying, Li, Lingmin, Wang, Yue, Yuan, Zeng, Zhang, Wenjing, Hatch, Kenneth, Zheng, Wenxin

January 2014

BACKGROUND:Serous tubal intraepithelial carcinoma (STIC) and the p53 signature in tubal mucosa have been supported to be precursor lesions in high-grade serous carcinoma (HGSC) of the fallopian tube, ovary, and peritoneum. It remains critical to find biomarkers for precursor lesions in order to detect HGSCs efficiently. IMP3 is an oncoprotein that has been explored in human malignancies. No studies have specifically addressed the expression of IMP3 in precursor or early lesions of HGSC. The main purposes of this study are to evaluate if IMP3 plays any role in the process of pelvic serous carcinogenesis by examining its expression in HGSC precursor lesions, to examine the relationship between IMP3 and p53 in those precursor lesions, and to check if IMP3 can be used as a biomarker for early diagnosis.METHODS:Immunohistochemistry for IMP3 and p53 was performed and evaluated in 48 HGSCs with STIC, 62 HGSCs without STIC, and 60 benign cases as negative controls. Sections of fallopian tubes with or without STIC , as well as cancers within the ovaries, were studied. IMP3 signature was defined as strong IMP3 cytoplasmic staining in 10 or more consecutive benign-looking tubal epithelial cells. The relationship between IMP3 and p53 overexpression was examined.RESULTS:In the 48 HGSC patients with STIC, IMP3 was positive in 46% of STIC lesions and had a similar positive rate in the invasive components of HGSC. IMP3 was also expressed in normal appearing tubal epithelia (IMP3 signature) in 15 (31%) of 48 HGSC cases with STIC and 10 (16%) of 62 cases without STIC. In contrast, no single IMP3 signature was found in the benign control group. Concordant expression of IMP3 and p53 signatures in the STIC group was found in up to one-third of the cases. There were also five (10%) STIC cases with positive IMP3 and negative p53.CONCLUSIONS:We conclude that IMP3 may be involved in the process and progression of pelvic HGSC and may serve as a complimentary biomarker in diagnosing STIC.

IMP3

Serous tubal intraepithelial carcinoma

STIC

p53 signature

High-grade serous carcinoma

Cytologic studies of the fallopian tube in patients undergoing salpingo-oophorectomy

Chen, Hao, Klein, Robert, Arnold, Stacy, Chambers, Setsuko, Zheng, Wenxin

01 October 2016

Background: Mounting evidence suggests the fallopian tube as the origin for ovarian high grade serous carcinoma (HGSC). We attempted to identify the tubal cytological features that allow us to distinguish malignant from benign conditions. Methods: Tubal specimens (n = 56) were collected from patients who underwent bilateral salpingo-oophorectomy (BSO) due to various clinical indications. A standard procedure to collect fallopian tube brushings from freshly received surgical specimens was developed. Cytological diagnoses were classified into three categories: benign, atypical, and suspicious for malignancy/malignant. Cytological variables of individual cells and epithelia were subjected to statistical analysis. The fallopian tube histology was used as diagnostic reference for confirmation of cytology diagnosis. Results: Among the 56 fallopian tube specimens, 2 (3.7 %) showed inadequate cellularity preventing further evaluation, 11 (20.4 %) were diagnosed as malignant or suspicious of malignancy, 7 were atypical, and 36 were benign. The presence of three dimensional clusters (p < 0.0001, Fisher's Exact Test), or prominent nucleoli (p = 0.0252, Fisher Exact test) was highly correlated with the diagnosis of malignancy. The suspicious malignant/malignant cytological diagnosis was also highly correlated with presence of HGSC with or without serous tubal intraepithelial carcinoma (STIC). Conclusions: Tubal cytology may be useful for ovarian cancer screening and early detection.

Tubal cytology

High-grade serous carcinoma

Serous tubal intraepithelial carcinoma

Early detection

Atypical cytology

Ovarian serous carcinoma: recent concepts on its origin and carcinogenesis

Li, Jie, Fadare, Oluwole, Xiang, Li, Kong, Beihua, Zheng, Wenxin

January 2012

Recent morphologic and molecular genetic studies have led to a paradigm shift in our conceptualization of the carcinogenesis and histogenesis of pelvic (non-uterine) serous carcinomas. It appears that both low-grade and high-grade pelvic serous carcinomas that have traditionally been classified as ovarian in origin, actually originate, at least in a significant subset, from the distal fallopian tube. Clonal expansions of the tubal secretory cell probably give rise to serous carcinomas, and the degree of ciliated conversion is a function of the degree to which the genetic hits deregulate normal differentiation. In this article, the authors review the evidentiary basis for aforementioned paradigm shift, as well as its potential clinical implications.

Ovarian cancer

Fallopian tube

Carcinogenesis

Serous carcinoma

p53 signatures

Overexpression and oncogenic function of HMGA2 in endometrial serous carcinogenesis

Wei, Linxuan, Liu, Xiaolin, Zhang, Wenjing, Wei, Yuyan, Li, Yingwei, Zhang, Qing, Dong, Ruifen, Kwon, Jungeun Sarah, Liu, Zhaojian, Zheng, Wenxin, Kong, Beihua

January 2016

The high-mobility group A protein 2 (HMGA2) is a non-histone chromatin factor highly expressed in fetal tissue and malignant tumors but rarely detected within normal adult tissues. The clinical implications and biological functions of HMGA2 in endometrial carcinoma are largely unknown. Here we report that HMGA2 expression was barely detected in benign endometrium samples (2 of 28 samples). However, HMGA2 expression increased significantly from precancerous lesion endometrial glandular dysplasia (7 of 17, 41.2%), to serous endometrial intraepithelial carcinoma (5 of 8, 62.5%) and to full blown endometrial serous carcinoma (39 of 59, 66.1%). Functional characterization of HMGA2 revealed that the gene has both tumor growth promotion and metastasis. In addition, HMGA2 induced epithelial-mesenchymal transition (EMT) through modulation vimentin and β-catenin. Furthermore, HMGA2 overexpression started from endometrial serous precancers, non-invasive cancers, as well as in full blown carcinomas in a p53 knockout mouse model we recently established in our laboratory. Our findings suggest that HMGA2 may serve as a useful diagnostic marker in the assessment of endometrial serous cancer and its precursor lesions.

HMGA2

endometrial serous carcinoma

tumor growth

metastasis

EMT

The effect of normobaric hyperoxia on patients with central serous chorioretinopathy

Najem, Mortada Salman

29 November 2021

PURPOSE: Normobaric hyperoxia (NBH) has been shown in animal models of experimental retinal detachment (RD) to effectively prevent photoreceptor degeneration. Furthermore, choroidal hyperpermeability has been implicated in the disease pathophysiology. In this study, we studied the effects of 3-hours of 40% FIO2 NBH on photoreceptor morphology and visual acuity in patients with vision loss associated with active central serous chorioretinopathy (CSCR). MATERIALS and METHODS: A total of 8 patients with active unilateral CSCR received at least one 3-hour NBH (40% FIO2) session. Best corrected visual acuity (BCVA) as well as thickness of the central macula, subretinal fluid (SRF), photoreceptor layer (PL), and outer nuclear layer (ONL) were assessed. RESULTS: In patients with unilateral acute CSCR, 3 hours of 40% FIO2 NBH showed a trend towards improved vision, but no statistical differences were obtained for BCVA, CMT, SRF, PL, or ONL. CONCLUSIONS: Administration of 3-hours of NBH did not induce any measurable anatomic changes in the retina nor any significant changes in visual acuity. These results challenge the hypothesis of choroidal hyperpermeability in CSCR and suggest that additional or alternative pathologies contribute to this disease. / 2022-11-29T00:00:00Z

Ophthalmology

Central serous chorioretinopathy

Exudative

Hyperoxia

Non-rhegmatogenous

Retina

Retinal detachment

Borderline Tumors of the Ovary: A Clinicopathological Study

Yasmeen, Samia, Hannan, Abdul, Sheikh, Fareeha, Syed, Amir Ali, Siddiqui, Neelam

01 March 2017

Objective: To report experience with borderline ovarian tumors (BOTs) in a developing country like Pakistan with limited resources and weak database of health system. Methods: Patients with BOTs managed at Shaukat Khanum Cancer hospital, Lahore, Pakistan from 2004 to 2014 were included and reviewed retrospectively. Data was recorded on histopathological types, age, CA-125, stage of disease, treatment modalities and outcomes. Results: Eighty-six patients with BOT were included with a median age of 35 years. Forty-two (49%) patients had serous BOTs and 43 (50%) had mucinous BOTs, while one (1%) had mixed type. Using FIGO staging, 80 patients had stage I; two patients had IIA, IIB and stage III each. Median follow-up time was 31.5 months. All patients had primary surgery. Seventy (81%) patients underwent complete surgical resection of tumor. Forty-three (50%) patients had fertility preserving surgery. Seventy-three (85%) patients remained in remission. Recurrent disease was observed in 13 (15%) patients. Median time to recurrence was 22 months. On further analysis, age above forty years, late stage at diagnosis and incomplete surgery were significantly associated with invasive recurrence. Conclusion: Despite a low malignant potential, relapses may occur in patients above forty years of age, incomplete surgery and staging information and advanced stage at presentation. Fertility sparing surgery should be considered in young patients. Complete excision of tumor and prolonged follow-up are advised because recurrence and transformation to invasive carcinoma may occur.

borderline ovarian tumor

FIGO

mucinous ovarian tumor

serous ovarian tumor

Rôles de CXCL12beta dans l'hétérogénéité fibroblastique et l'immunosuppression dans les cancers de l'ovaire / Roles of CXCL12 beta in fibroblastic heterogeneity and immunosuppression in ovarian cancers

Givel, Anne-Marie

13 September 2016

Les cancers épithéliaux de l’ovaire sont la première cause de décès par cancer gynécologique. Dans ce travail, nous nous sommes intéressés aux cancers ovariens séreux de haut grade (HGSOC) et de stade avancé, pour lesquels les options thérapeutiques demeurent limitées. Plusieurs laboratoires, dont le nôtre, ont identifié des groupes moléculaires distincts au sein de ces HGSOC sur la base de données transcriptomiques.Dans toutes ces études, un sous-groupe moléculaire, nommé « fibrose » ou« mésenchymateux », est systématiquement observé et invariablement associé à un pronostic sombre pour les patientes. La signature transcriptomique qui identifie ce groupe de patientes inclue de nombreux gènes impliqués dans le remodelage de la matrice extracellulaire et la composition stromale, suggérant un rôle possible du stroma dans l’agressivité de ce sous-groupe moléculaire particulier d’HGSOC.Par une étude combinant de façon originale l’analyse concomitante de 6 marqueurs de fibroblastes associés au cancer (CAF), nous mettons en évidence pour la première fois l’existence de 4 sous-populations de CAF. De façon intéressante, l’une de ces 4 populations(dite CAF-S1) s’accumule significativement dans le sous-type moléculaire« fibrose/mésenchymateux » des HGSOC. Or, cette population particulière de CAF-S1 présente une activité immunosuppressive, en favorisant non seulement la survie ou l’attraction des lymphocytes T régulateurs, mais également en stimulant leur activation par l’expression du facteur de transcription FOXP3 (Forkhead Box P3). Enfin, nous identifions l’isoforme β de CXCL12 (chimiokine à motif C-X-C ligand 12) comme un acteur majeur de l’identité et de la fonctionnalité de ces CAF-S1 immunosuppresseurs. En effet, CXCL12βs’accumule spécifiquement dans les CAF-S1 et joue un rôle clé dans la fonction immunosuppressive de ces CAF au sein du stroma des HGSOC mésenchymateux.Nos résultats mettent ainsi en évidence un mécanisme expliquant, au moins en partie, le pronostic sombre des patientes atteintes d’HGSOC mésenchymateux. La caractérisation approfondie du stroma de ces tumeurs agressives permet d’envisager de nouvelles stratégies thérapeutiques ciblant à la fois les CAF et les cellules immunitaires dans le but d’améliorer la survie des patientes mésenchymateuses. / Epithelial ovarian cancers are the first cause of death from gynecologic cancer. We focusedour work on high-grade serous ovarian cancer (HGSOC) patients, for who only very fewtherapeutic options exist. In the past, several laboratories, including ours, have identified -based on transcriptomic data- distinct molecular subgroups amongst HGSOC. Interestingly,among these different molecular subgroups, one of them, referred to as “Fibrosis” or“Mesenchymal” is systematically identified and consistently associated with poor patientprognosis in all studies. Transcriptomic signature that defines this specific molecularsubgroup of HGSOC contains mainly genes involved in extracellular matrix remodeling andstromal composition, suggesting a potential role of stroma and Carcinoma-AssociatedFibroblasts (CAF) in this particular “Fibrosis/Mesenchymal” HGSOC subgroup.By combining various technics studying concomitantly 6 different CAF markers, we identifiedfor the first time 4 different subpopulations of CAF in HGSOC. Interestingly, one of thesesub-populations, referred to as CAF-S1, significantly accumulates in the“Mesenchymal/Fibrosis” subgroup of HGSOC. Importantly, we demonstrated that the CAFS1cellular subpopulation exhibits immunosuppressive activities. Indeed, CAF-S1 fibroblastsnot only by attract regulatory T lymphocytes but also promote their survival and activation(assessed by expression of FOXP3). Finally, we uncovered the specific role of the CXCL12βisoform as an important player of CAF-S1 identity and immunosuppressive functions inmesenchymal HGSOC.All together, these results identify a stromal heterogeneity in HGSOC, which has beenbroadly underestimated until now. Moreover, our work demonstrates the accumulation of aCAF subpopulation with immunosuppressive functions in HGSOC mesenchymal patients thatcould account, at least in part, for their poor survival rate. Deep characterization of thestroma may enable us to define new therapeutic options combining CAF-targeting therapiesand immunotherapies, in order to improve survival of HGSOC mesenchymal patients.

Cancers ovariens séreux

FOXP3

Serous ovarian cancers

FOXP3

The BMP signaling pathway leads to enhanced proliferation in serous　ovarian cancer-A potential therapeutic target / BMPシグナル伝達経路は卵巣漿液性腺癌の細胞増殖を促進させ、新規治療標的となりうる

Peng, Jin

23 March 2015

京都大学 / 0048 / 新制・課程博士 / 博士(医学) / 甲第18895号 / 医博第4006号 / 新制||医||1009(附属図書館) / 31846 / 京都大学大学院医学研究科医学専攻 / (主査)教授 松田 道行, 教授 武藤 学, 教授 戸口田 淳也 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

BMP: bone morphogenetic protein

SMAD

serous ovarian cancer

490

Immunosuppressive tumor microenvironment in Uterine Serous Carcinoma via CCL7 signal with myeloid-derived suppressor cells / 子宮体部漿液性癌における骨髄由来抑制細胞とCCL7シグナルを介した免疫抑制性腫瘍微小環境の解明

Mise, Yuka

24 November 2022

京都大学 / 新制・課程博士 / 博士(医学) / 甲第24284号 / 医博第4900号 / 新制||医||1061(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 羽賀 博典, 教授 上野 英樹, 教授 髙折 晃史 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

Uterine serous carcinoma

MDSC

tumor microenvironment

Ccl7

tumor immunity

490