immunosuppression complications

  • 文章类型: Case Reports
    溃疡性结肠炎(UC)是炎症性肠病的一种亚型,可导致大肠衬里的炎症和溃疡。UC患者经常服用免疫抑制药物来治疗他们的症状,导致许多潜伏病毒重新激活的风险增加,包括单纯疱疹病毒(HSV)和巨细胞病毒(CMV)。然而,患者很少同时出现两种病毒的再激活。这里,我们记录演示文稿,医院课程,1例HSV和CMV双重感染的UC患者的临床表现。我们还描述了管理双重感染的治疗策略和预防措施。这可以通过在诊断后的门诊环境中开始使用伐更昔洛韦来观察。
    Ulcerative colitis (UC) is a subtype of inflammatory bowel disease that results in inflammation and ulceration in the lining of the large intestine. Patients with UC are frequently prescribed immunosuppressive medications to treat their symptoms, resulting in an increased risk of reactivation of many latent viruses, including herpes simplex virus (HSV) and cytomegalovirus (CMV). However, it is rare for a patient to present with simultaneous reactivation of both viruses. Here, we document the presentation, hospital course, and clinical findings of a UC patient with HSV and CMV dual infection. We also describe treatment strategies and prophylactic measures for managing a dual infection. This is seen through initiating valganciclovir in the outpatient setting following the diagnosis.
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  • 文章类型: Case Reports
    已经在多器官系统中描述了移植后患者的腺病毒感染,最经典的是肺,肝脏,和消化道。在泌尿生殖道,出血性膀胱炎是最常见的。临床上明显的肾受累腺病毒是罕见的,腺病毒相关性间质性肾炎(AAIN)是肾移植失败的罕见原因。这里,我们介绍了三例AAIN患者,在及时诊断和治疗调整后,经历了同种异体移植功能的恢复。所有患者均接受标准三联疗法,活检时他克莫司水平在目标范围内。没有病人有呼吸道症状,尽管腹泻,结肠活检为阴性。只有1例腺病毒血清学阳性(仅IgG),3例尿液阳性;两名患者白细胞减少,无中性粒细胞减少。肾活检显示特征性的肉芽肿性肾小管中心混合淋巴细胞和中性粒细胞浸润。腺病毒免疫组织化学(IHC)在肾小管上皮(细胞核和细胞质)中显示强染色,而多瘤病毒染色为阴性。一名患者在诊断为AAIN后两个月进行的随访活检显示持续的细胞病变作用,腺病毒IHC染色阴性,而另一名患者在一年时进行的活检显示肾小球和肾小管间质瘢痕形成。在急性肾移植功能障碍的情况下,AAIN是一种不常见但重要的病因。尽管AAIN的症状是非特异性的,经常注意到血尿。对于伴有坏死和混合炎症浸润的肉芽肿性炎症的病例,应考虑腺病毒IHC。正如这个单一机构案例系列所表明的那样,及时诊断可导致移植肾的保存。有病史的患者也应考虑腺病毒感染后的持续细胞病变效应。或潜在的历史,AAIN。
    Adenoviral infections in post-transplant patients have been described in multiple organ systems, most classically the lung, liver, and alimentary tract. In the genitourinary tract, hemorrhagic cystitis is most frequently observed. Clinically apparent renal involvement with adenovirus is rare, and adenovirus-associated interstitial nephritis (AAIN) is an uncommon cause of renal allograft failure. Here, we present three cases of AAIN in patients who, after prompt diagnosis and treatment adjustment, experienced a return of allograft function. All patients were on standard triple therapy with tacrolimus levels within the target range at the time of biopsy. None of the patients had respiratory symptoms, and despite diarrhea, colon biopsies were negative. Only case one had positive adenovirus serology (IgG only) and case three had positive urine; two patients had leukopenia without neutropenia. Renal biopsies showed a characteristic granulomatous tubulocentric mixed lymphocytic and neutrophilic infiltrate. Adenovirus immunohistochemistry (IHC) showed strong staining in the tubular epithelium (nuclear and cytoplasmic) while staining for polyomavirus was negative. A follow-up biopsy two months after the diagnosis of AAIN in one patient revealed persistent cytopathic effects with negative adenoviral IHC staining while a biopsy at one year in another patient showed glomerular and tubulointerstitial scarring. AAIN is an uncommon but important etiology to consider in cases of acute renal allograft dysfunction. Although the presenting symptoms for AAIN are nonspecific, hematuria is frequently noted. Adenovirus IHC should be considered in cases with granulomatous inflammation associated with necrosis and mixed inflammatory infiltrate. As demonstrated in this single-institution case series, prompt diagnosis can result in the preservation of the renal allograft. Lasting cytopathic effects after adenoviral infection should also be considered in patients with a history, or potential history, of AAIN.
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