key: cord-1001192-a51syanm
authors: Ali, Hatem; Daoud, Ahmed; Mohamed, Mahmoud M.; Salim, Sohail Abdul; Yessayan, Lenar; Baharani, Jyoti; Murtaza, Asam; Rao, Vinaya; Soliman, Karim M.
title: Survival rate in acute kidney injury superimposed COVID-19 patients: a systematic review and meta-analysis
date: 2020-04-27
journal: Ren Fail
DOI: 10.1080/0886022x.2020.1756323
sha: 44eb2f83d8c9c7d9a8da820f39c5dcbcabaa7ba6
doc_id: 1001192
cord_uid: a51syanm

nan

Dear Editor, Of no doubt, the whole world is passing through a potentially life-threatening and economically destructive global pandemic caused by the novel coronavirus (COVID-19; SARS-CoV-2; previously known as 2019-nCoV) [1] . The clinical course of infection is widely unpredicted and variable, ranging from asymptomatic infection to multi-organ system failure and death [2] [3] [4] . Nevertheless, the survival rate among patients with COVID-19 and superimposed acute kidney injury (AKI) remains unclear [5, 6] . Hence; we ushered a systemic review and meta-analysis exploring the survival outcome of COVID-19 subjects who developed severe AKI, the latter defined as subjects who require acute renal replacement therapy (RRT) or meet the Kidney Disease Improving Global Outcome (KDIGO) definition of AKI stage III. We included all studies performed on human beings for which baseline creatinine, occurrence of AKI stage III and/or need for acute RRT were reported and excluded case reports, review articles, or studies assessing clinical characteristics and conference abstracts. Ethical approval was not required for this work due to use of anonymous data that is publicly available. A systematic review in Pubmed, Medline, Embase and Cochrane databases to select studies that met the inclusion criteria was performed by 3 authors (H.A, M.M, A.A). The search terms used were (coronavirus, COVID-19, SARS-COV-2 and (mortality, survival, outcomes, dialysis, acute renal failure, acute kidney injury, renal replacement therapy). These search terms were individually used and then combined in different databases. References within the chosen studies were reviewed. All the included studies were reviewed by supervising authors. Any disagreement among authors collecting the data was investigated by supervising authors. Consensus among all authors was essential to include the studies in the systematic review. The following data were collected: name of the first author, journal title, publication date, place of the study, sample size, baseline creatinine, relative risk and confidence intervals for association of acute renal failure and mortality. We followed the recommendations of Cochrane collaboration and the Quality of Reporting of Meta-analyses guidelines [7, 8] . STATA package-15 was used for statistical analysis. We combined all study-specific estimates using inverse-variant weighted averages of logarithmic relative risk in random effects model (REM). Confidence interval including the value of one was used evident for statistically significant estimate.

Heterogeneity was evaluated using Higgins I-squared statistic. Heterogeneity was estimated when the level of p value was <.1. Results of the REM were spread out on the forest plot graph. The Newcastle-Ottawa score was used to evaluate the quality of the papers included. Egger's test was used to assess publication bias. A total of 2290 abstracts were reviewed. Out of six studies included in the systematic review, only three studies met the inclusion criteria and were pooled into a meta-analysis (PRISMA diagram, Figure 1 ). Due to lack of a controlled survival group (only severe AKI subjects were included), the studies by Zhang et al. and Shi et al. were not included in the metaanalysis [9, 10] . As compared to Ruan et al., Cheng et al.'s study was more recent, included a larger sample size and since both shared the same cohort, only the latter was included in our meta-analysis [5, 11] . The baseline characteristics of the studies included are shown in Table 1 . The Newcastle-Ottawa score of the included studies is shown in Table 2 . REM showed that severe AKI is associated with higher risk of mortality (relative risk ¼ 3.08, confidence interval ranges from 1.54 to 6.19) as shown in Figure 2 . There was evidence of heterogeneity with I-squared ¼90% and p < .001. Publication bias was shown in the funnel plot analysis in Figure 3 . By applying Egger's test for assessment of bias, there was evidence of small studies effect with p ¼ .93.

To decrease risk of heterogeneity, REM was repeated after excluding Yang et al ( Figure 4 ). The association of severe AKI with mortality persisted (relative risk ¼ 4.19, 95% CI 3.31 -5.31). There was no evidence of heterogeneity with I-squared ¼ 0%, p ¼ .68. There was no evidence of publication bias when applying Eggers test (p < .05) or funnel plot analysis ( Figure 5 ). Our meta-analysis supports that mortality is significantly higher in patients with severe AKI in patients with COVID-19. To date, the published incidence of AKI among patients with COVID-19 is highly variable. It has been reported to occur in up to 27% of patients with COVID-19 [12] . Our meta-analysis included three studies addressing mortality in COVID-19 patients with superimposed AKI. Cheng et al., included 701 COVID-19 confirmed cases. AKI stage III occurred among 14/701 (2%) of the patients and was associated with an increased risk of in-hospital mortality (hazard ratio ¼ 9.81, 95% CI:5.46-17.65) [5] . Similarly, Yang et al. included 52 COVID-19 confirmed cases in their study and found that 8 out of 9 subjects who required RRT did not survive [13] . Mirroring Yang et al.'s results, Zhou et al., in a study that included 191 COVID-19-CC, 10 out of 10 subjects who required RRT did not survive [14] . In addition, the investigators reported that out of 33 confirmed COVID-19 cases who developed AKI, 32 patients did not survive [14] . The high mortality in COVID-19 patients and severe AKI, even with RRT, could be due to the kidney-lung crosstalk during COVID-19 infection and amplification of inflammation during AKI in a cohort with high incidence of acute respiratory distress syndrome [15] . Based on the available limited published data, severe AKI in patients with COVID-19 is an ominous clinical predictor and is associated with high mortality.

Further studies are needed to understand the factors associated with worse outcomes among COVID-19 patients with AKI. Understanding those factors may guide care providers in making more informed dialysis eligibility decisions under conditions where resources are extremely limited. 

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The authors declare no conflicts of interest.