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狼疮性肾炎重复肾活检的预后意义:组织病理学恶化以及两次活检之间的时间间隔短与终末期肾病和死亡风险显著增加相关。

Prognostic significance of repeat biopsy in lupus nephritis: Histopathologic worsening and a short time between biopsies is associated with significantly increased risk for end stage renal disease and death.

作者信息

Arriens Cristina, Chen Sixia, Karp David R, Saxena Ramesh, Sambandam Kamalanathan, Chakravarty Eliza, James Judith A, Merrill Joan T

机构信息

Oklahoma Medical Research Foundation, 825 NE 13th Street, Oklahoma City, OK 73104, United States.

University of Oklahoma Health Sciences Center, 801 NE 13th Street, Oklahoma City, OK 73104, United States.

出版信息

Clin Immunol. 2017 Dec;185:3-9. doi: 10.1016/j.clim.2016.11.019. Epub 2016 Dec 3.

Abstract

BACKGROUND/PURPOSE: Approximately half of patients with systemic lupus erythematosus (SLE) develop lupus nephritis (LN), a major cause of morbidity and early mortality in that disease. Prolonged renal inflammation is associated with irreversible kidney damage which confers a 30% risk of end stage renal disease (ESRD), making early, aggressive treatment mandatory. Failure to achieve therapeutic response or recurrence of renal flare often prompts repeat biopsy. However, the role of repeat biopsy in determining long-term renal prognosis remains controversial. For this reason repeat biopsies are usually not utilized unless clinical evidence of refractory or recurrent disease is already present, despite known mismatches between clinical and biopsy findings. The current study quantifies the degree to which histopathologic worsening between first and second biopsies and duration between them predicts ESRD and death.

METHODS

Medical records of 141 LN patients with more than one biopsy were obtained from a single large urban medical center. Cases were attained using billing codes for diagnosis and procedures from 1/1999-1/2015. Biopsy worsening was defined as unfavorable histopathologic classification transitions and/or increased chronicity; if neither were present, the patient was defined as non-worsening. We used Cox proportional hazard models to study the relationship between ESRD and survival adjusting for covariates which included age at first biopsy, gender, race, initial biopsy class, and initial induction therapy.

RESULTS

Of 630 patients screened, 141 had more than one biopsy. Advancing chronicity was detected in 48 (34.0%) and a renal class switch to worse grade of pathology was found in 54 (38.3%). At least one of these adverse second biopsy features was reported in 79 (56.0%) patients. Five years following initial biopsy, 28 (35.4%) of those with worsening histopathology on second biopsy developed ESRD, compared to 6 (9.7%) of non-worsening patients and 10 (12.7%) of patients with worsening histopathology had died compared to 2 (3.2%) of non-worsening patients. Biopsy worsening was associated with a significantly greater 15-year risk of ESRD (Hazard Ratio 4.2, p=0.0001) and death (Hazard Ratio 4.3, p=0.022), adjusting for age, gender, race, biopsy class, and treatment. Time between first and second biopsies was <1year in 32 patients, 1-5years in 81, and >5years in 28. Over a 15-year period, those with <1year between first and second biopsies (presumably enriched for patients with early clinical signs of progression) had a significantly greater risk of ESRD (Hazard Ratio 13.7, p<0.0001) and death (Hazard Ratio 16.9, p=0.0022) after adjusting for age, gender, race, biopsy class, and treatment.

CONCLUSION

A repeat renal biopsy demonstrating worsening pathology increases the risk of ESRD and death more than four-fold compared to non-worsening patients. Given known potential mismatch between biopsy and clinical data, repeat biopsies may add important information and justify changes in treatment not considered on clinical grounds. Earlier detection of poor prognostic signs in those without early clinical deterioration might improve outcomes in enough patients to reconsider cost effectiveness of routine repeat biopsy.

摘要

背景/目的:约半数系统性红斑狼疮(SLE)患者会发展为狼疮性肾炎(LN),这是该疾病发病和早期死亡的主要原因。长期的肾脏炎症与不可逆的肾脏损伤相关,会使患者有30%的风险发展为终末期肾病(ESRD),因此必须尽早进行积极治疗。未能实现治疗反应或肾脏炎症复发常常促使再次进行活检。然而,再次活检在确定长期肾脏预后方面的作用仍存在争议。因此,除非已有难治性或复发性疾病的临床证据,尽管已知临床和活检结果存在不匹配,通常也不会进行再次活检。本研究量化了首次活检与第二次活检之间组织病理学恶化的程度以及两次活检之间的时间间隔对ESRD和死亡的预测作用。

方法

从一个大型城市医疗中心获取了141例接受过不止一次活检的LN患者的病历记录。通过1999年1月至2015年1月期间的诊断和操作计费代码来确定病例。活检恶化被定义为组织病理学分类转为不利情况和/或慢性化增加;如果两者均未出现,则患者被定义为未恶化。我们使用Cox比例风险模型来研究ESRD与生存之间的关系,并对协变量进行了调整,协变量包括首次活检时的年龄、性别、种族、初始活检类别和初始诱导治疗。

结果

在筛查的630例患者中,141例接受过不止一次活检。48例(34.0%)出现慢性化进展,54例(38.3%)肾脏病理分级转为更差级别。79例(56.0%)患者报告了至少一项这些不利的第二次活检特征。首次活检后5年时,第二次活检组织病理学恶化的患者中有28例(35.4%)发展为ESRD,而未恶化患者中为6例(9.7%);第二次活检组织病理学恶化的患者中有10例(12.7%)死亡,而未恶化患者中为2例(3.2%)。在对年龄、性别、种族、活检类别和治疗进行调整后,活检恶化与15年ESRD风险显著增加相关(风险比4.2,p = 0.0001)以及与死亡风险显著增加相关(风险比4.3,p = 0.022)。首次活检与第二次活检之间的时间间隔在32例患者中<1年,81例患者中为1 - 5年以及28例患者中>5年。在15年期间,首次活检与第二次活检之间时间间隔<1年的患者(可能富集了具有早期临床进展迹象的患者)在对年龄、性别、种族、活检类别和治疗进行调整后,ESRD风险显著增加(风险比13.7,p < 0.0001)以及死亡风险显著增加(风险比16.9,p = 0.0022)。

结论

与未恶化的患者相比,再次肾脏活检显示病理恶化会使ESRD和死亡风险增加四倍以上。鉴于已知活检与临床数据之间可能存在不匹配,再次活检可能会提供重要信息,并证明基于临床理由未考虑的治疗改变是合理的。在那些没有早期临床恶化的患者中更早地发现不良预后迹象可能会改善足够多患者的结局,从而重新考虑常规再次活检的成本效益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/93e9/5457715/183af41e26f5/nihms837461f1.jpg

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