Kaposi’s sarcoma manifested as lower gastrointestinal bleeding in a HIV/HBV-co-infected liver cirrhosis patient: A case report

BACKGROUND Kaposi’s sarcoma(KS)is one of the most common cancers in human immunodeficiency virus(HIV)-positive patients and leads to a high prevalence of morbidity and mortality.It usually appears as cutaneous or mucous lesions.Patients with visceral KS are asymptomatic and clinically silent.As the disease advances,patients may progress from a normal condition to exhibiting severe symptoms.CASE SUMMARY A 27-year-old man presented with a 2-mo history of fever,bearing-down pain,and rectal bleeding.His hepatitis B virus DNA level was 2.7×107 IU/mL.Abdominal computed tomography(CT)indicated liver cirrhosis.Before he was admitted to our hospital,he was diagnosed with HIV infection.His CD4 count was 24 cells/μL.Pelvic cavity CT suggested a thickened rectum wall accompanied by multiple enlarged lymph nodes.The patient was initially treated as having haemorrhoidal varices with bleeding,telbivudine for anti-hepatitis B virus treatment,and antibiotics for anti-infection.After half a month of treatment,the patient felt that his lower lumbus ache and bearing-down pain had not improved,and a colonoscopy was conducted.The result revealed a rectal mass that was histologically confirmed as KS with rectal spindle cells that were positive for cluster of differentiation 117(CD117),CD34,human herpes virus 8,and CD31.He was administered systemic chemotherapy with 36 mg/d liposomal doxorubicin six times.The patient experienced no sign of lower gastrointestinal bleeding again.CONCLUSION This case highlights the diagnosis of primary KS with lower gastrointestinal bleeding in HIV-positive patients,which means visceral KS could not be excluded.The gold standard relies on colonoscopy and biopsy findings.

Intestinal Kaposi's sarcoma may mimic gastrointestinal stromal tumor in HIV infection

Diffuse intestinal Kaposi＇s sarcoma shares macroscopic and histopathologic features with gastrointestinal stromal tumors. Correct diagnosis may pose a clinical challenge. We describe the case of a young HIV-1-infected African lady without advanced immunodeficiency, who presented with a diffuse spindle cell tumor of the gut. Initial diagnosis was of a gastrointestinal stromal tumor, based on endoscopy and histopathology. Further evaluation revealed evidence for human herpesvirus 8 （HHV8） and the diagnosis had to be changed to diffuse intestinal Kaposi＇s sarcoma. Antiretroviral triple therapy together with chemotherapy was commenced, and has led to the rapid remission of intestinal lesions. With a background of HIV infection, the presence of HHV8 as the causative agent of Kaposi＇s sarcoma should be determined, as distinct treatment is indicated.

Diagnostic value of endothelial markers and HHV-8 staining in gastrointestinal Kaposi sarcoma and its difference in endoscopic tumor staging

AIM: To clarify the diagnostic values of hematoxylin and eosin (HE), D2-40, CD31, CD34, and HHV-8 immunohistochemical (IHC) staining in gastrointestinal Kaposi's sarcoma (GI-KS) in relation to endoscopic tumor staging. METHODS: Biopsy samples (n = 133) from 41 human immunodeficiency virus-infected patients were reviewed. GI-KS was defined as histologically negative for other GI diseases and as a positive clinical response to KS therapy. The receiver operating characteristic area under the curve (ROC-AUC) was compared in relation to lesion size, GI location, and macroscopic appearances on endoscopy. RESULTS: GI-KS was confirmed in 84 lesions (81.6%). Other endoscopic findings were polyps (n = 9), inflammation (n = 4), malignant lymphoma (n = 4), and condyloma (n = 2), which mimicked GI-KS on endoscopy. ROC-AUC of HE, D2-40, blood vessel markers, and HHV-8 showed results of 0.83, 0.89, 0.80, and 0.82, respectively. For IHC staining, the ROC-AUC of D2-40 was significantly higher (P < 0.05) than that of HE staining only. In the analysis of endoscopic appearance, the ROC-AUC of HE and IHC showed a tendency toward an increase in tumor staging (e.g. , small to large, patches, and polypoid to SMT appearance). D2-40 was significantly (P < 0.05) advantageous in the upper GI tract and for polypoid appearance compared with HE staining. CONCLUSION: The diagnostic value of endothelial markers and HHV-8 staining was found to be high, and its accuracy tended to increase with endoscopic tumor staging. D2-40 will be useful for complementing HE staining in the diagnosis of GI-KS, especially in the upper GI tract and for polypoid appearance.

Kaposi’s Disease (KS) in a Senegalese Child Living with HIV

Kaposi’s Disease or Kaposi’s Sarcoma (SK ) is a multifocal malignant proliferation induced by viral growth factors, including interleukin 6 of human herpes virus type 8 (HHV8). We describe four forms of this disease who poses a real public health problem in East and Central Africa. The purpose of our observation was to report a rare condition in a Senegalese HIV-positive child. It was an 11-year-old girl from a region in central Senegal. She was an orphan of both parents, tested and monitored since the age of 5 for HIV infection 1. She was on the 1st line protocol. Due to a lack of support and good observance, she was referred to us at the age of 11 for follow-up in our structure in the suburbs of Dakar. The initial follow-up assessment showed a very low CD4 count and a very high viral load. Before the lack of clinical and immune-virological response, a genotypic resistance test was performed and showed immunological and virological failure. The initial development was marked by the appearance of lesions which were highly suggestive of Kaposi’s disease. She was on 2nd line treatment. The histopathological aspect of cutaneous biopsy was very suggestive of Kaposi’s disease. The subsequent course after ART and bleomycin treatment was clinically marked by regression of skin lesions. Virologically, it was marked by a fall in the viral load. Immunologically there was a gradual recovery of CD4 levels which came back to normal. Our observation demonstrates that absence of effective antiretroviral therapy for HIV increases the risk to develop Kaposi’s sarcoma.

艾滋病并Kaposi肉瘤的X线胸片表现及其诊断价值

目的:探讨艾滋病(AIDS)最常见的相关性恶性肿瘤Kaposi肉瘤(KS)的胸部X线表现及其诊断价值。材料和方法:回顾性分析经临床和病理确诊为AIDS并发KS胸部侵犯的24例胸部X线平片的表现,对其X线表现进行分析并评估其诊断价值。结果:AIDS并发KS的胸部X线表现为间质型网织结节影(6/24例),片块状阴影(5/24例),肺门增大增浓和纵隔影增宽(10/24例),胸腔积液和心包积液(6/24例),机会性感染(6/24例),特异性感染(2/24例)。X线平片无明显异常发现(5/24例)。结论:AIDS并发KS的表现多种多样,诊断需紧密结合临床。

人类8型疱疹病毒与胃肠型HIV卡波西肉瘤组织ORF42、mTORC1表达相关性研究

目的探究胃肠型HIV卡波西肉瘤组织中人类8型疱疹病毒(HHV8)感染与ORF42、哺乳动物雷帕霉素靶蛋白复合物1(mTORC1)表达的关系。方法选取2015年9月至2019年9月新疆维吾尔自治区人民医院收治的艾滋病合并胃肠型卡波西肉瘤患者36例作为研究对象。留取入组患者卡波西肉瘤组织及瘤旁组织,采用免疫组织化学染色检测胃肠型HIV卡波西肉瘤组织及瘤旁组织中HHV8表达情况,Western blotting法检测ORF42、mTORC1蛋白表达水平,qRT-PCR法检测ORF42、mTORC1、血管内皮生长因子(VEGF)、白介素-6(IL-6)mRNA表达水平,Pearson法分析胃肠型HIV卡波西肉瘤组织中ORF42、mTORC1与VEGF、IL-6相关性。结果胃肠型HIV卡波西肉瘤组织中HHV8阳性率明显高于瘤旁组织(P<0.05)。胃肠型HIV卡波西肉瘤组织中ORF42、mTORC1蛋白及mRNA,VEGF、IL-6 mRNA表达水平明显高于瘤旁组织(P<0.05)。感染亚组卡波西肉瘤组织中ORF42、mTORC1蛋白及mRNA,VEGF、IL-6 mRNA表达水平明显高于未感染亚组(P<0.05)。胃肠型HIV卡波西肉瘤组织中ORF42、mTORC1 mRNA与VEGF、IL-6 mRNA表达水平均呈正相关(P<0.05)。结论胃肠型HIV卡波西肉瘤组织中HHV8感染率增加,可能通过激活ORF42、mTORC1表达促进肿瘤发生发展。

HIV-1假病毒的构建及对人原发性渗出性淋巴瘤细胞系的感染研究

目的:分离、克隆水泡性口炎病毒(vesicular stomatitis virus,VSV)的包膜糖蛋白(VSV-GP)编码基因,包装人类免疫缺陷病毒1型(human immunodeficiency virus-1,HIV-1)假病毒,并研究其对人原发性渗出性淋巴瘤细胞系BCBL-1细胞的感染状况。方法:根据GenBank登记的VSV-GP基因核苷酸序列设计1对PCR引物,其5′端分别引入HindⅢ和BamHⅠ酶切位点。以质粒pHCMV-G为模板,PCR扩增VSV-GP基因,经双酶切后定向克隆进真核表达载体pcDNA3.1(+)中,构建重组真核表达质粒pVSV-GP。重组质粒经酶切鉴定、核酸序列测定和分析后与含包装和复制功能缺陷的HIV-1基因组重组质粒pNL4-3.Luc.R-E-共转染人胚肾HEK293T细胞,收获细胞进行Western blot,检测HIV-1p24蛋白的表达;收获HIV-1假病毒感染BCBL-1细胞,进行虫荧光素酶(Luciferase)报告基因活性检测以及用ELISA的方法检测感染后细胞上清中HIV-1p24蛋白的含量。结果:PCR分离、克隆的VSV-GP序列全长1536bp,序列经过核酸分析证实;Western blot在HIV-1p24蛋白预期位置检测到特异性条带;HIV-1假病毒感染BCBL-1细胞后上清可以检测到HIV-1p24蛋白,并且测得Luciferase活性值较对照组显著增高(P<0.05)。结论:成功包装了HIV-1假病毒,并且该病毒可以感染BCBL-1细胞。

误诊为疖的艾滋病相关Kaposi肉瘤1例

患者男,40岁,汉族。下颌部红褐色结节2个月,无特殊自觉症状。外院曾诊断为"疖"欲行切开引流;门诊拟诊"下颌结节待查,不除外Kaposi肉瘤"。皮损组织病理示:表皮大致正常,真皮内大量的梭形细胞增生,其间呈血管样裂隙,裂隙内可见红细胞;免疫组化标记CD31(+),CD34(+)。诊断:Kaposi肉瘤。