Huanxi Zhang
Sun Yat-sen University
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Featured researches published by Huanxi Zhang.
PLOS ONE | 2016
Huanxi Zhang; Yitao Zheng; L. Liu; Qian Fu; Jun Li; Qingshan Huang; Huijiao Liu; Ronghai Deng; C. Wang
Background We combined the outcomes of all randomised controlled trials to investigate the safety and efficacy of steroid avoidance or withdrawal (SAW) regimens in paediatric kidney transplantation compared with steroid-based (SB) regimens. Methods A systematic literature search of PubMed, Embase, Cochrane Library, the trials registry and BIOSIS previews was performed. A change in the height standardised Z-score from baseline (ΔHSDS) and acute rejection were the primary endpoints. Results Eight reports from 5 randomised controlled trials were included, with a total of 528 patients. Sufficient evidence of a significant increase in the ΔHSDS was observed in the SAW group (mean difference (MD) = 0.38, 95% confidence interval (CI) 0.07–0.68, P = 0.01), particularly within the first year post-withdrawal (MD = 0.22, 95% CI 0.10–0.35, P = 0.0003) and in the prepubertal recipients (MD = 0.60, 95% CI 0.21–0.98, P = 0.002). There was no significant difference in the risk of acute rejection between the groups (relative risk = 1.04, 95% CI 0.80–1.36, P = 0.77). Conclusions The SAW regimen is justified in select paediatric renal allograft recipients because it provides significant benefits in post-transplant growth within the first year post-withdrawal with minimal effects on the risk of acute rejection, graft function, and graft and patient survival within 3 years post-withdrawal. These select paediatric recipients should have the following characteristics: prepubertal; Caucasian; with primary disease not related to immunological factors; de novo kidney transplant recipient; with low panel reactive antibody.
Pediatric Transplantation | 2017
Hong-yang Wang; Jun Li; L. Liu; R. Deng; Qian Fu; Dicken S.C. Ko; Huanxi Zhang; S. Deng; C. Wang
Early graft loss and poor graft function limit the use of kidneys from infant donors. Six en bloc kidney transplantations were performed from infant donors younger than 10 months into pediatric recipients between November 2012 and September 2015 at our center. We retrospectively analyzed recipient and donor demographics, surgery procedures, complications, graft function and size, and patient and graft survival with a follow‐up of 6‐39 months (median 15.5 months). Donor age ranged from 1 to 10 months with weight ranging from 3.5 to 10 kg. Recipient age ranged from 10 to 16 years with weight ranging from 30 to 39 kg. One kidney was removed due to arterial thrombosis during surgery, while the other kidney of this en bloc graft remained viable. Urine leak followed by bilateral ureteral obstruction occurred in one recipient. All of the recipients showed immediate graft function. The size of the en bloc kidney increased from 4.2±0.6 cm to 7.6±0.6 cm 6 months after surgery. Patient and graft survival were both 100% at the last follow‐up. Our results show that en bloc kidney transplantation from infant donors younger than 10 months into pediatric recipients is effective under the condition of experienced surgical techniques and perioperative management.
Scientific Reports | 2017
Yifu Li; Yunyi Xiong; Huanxi Zhang; Jun Li; Dong Wang; Wenfang Chen; Xiaopeng Yuan; Qiao Su; Wenwen Li; Huiting Huang; Zirong Bi; L. Liu; C. Wang
This study aimed to investigate the protective effects of EGb761, a Ginkgo Biloba extract, against brain death-induced kidney injury. Sixty male Sprague Dawley rats were randomly divided into six groups: sham, brain-death (BD), BD + EGb b48h (48 hours before BD), BD + EGb 2 h (2 hours after BD), BD + EGb 1 h, and BD + EGb 0.5 h. Six hours after BD, serum sample and kidney tissues were collected for analyses. The levels of blood urea nitrogen (BUN) and serum creatinine significantly elevated in the BD group than in sham group. In all the EGb761-treated BD animals except for the BD + Gb 2 h group, the levels of BUN and serum creatinine significantly reduced (all P < 0.01). EGb761 attenuated tubular injury and lowered the histological score. In addition, the longer duration of drug treatment was, the better protective efficacy could be observed. EGb761 significantly reduced IL-1β, IL-6, TNF-α, MCP-1, IP-10 mRNA expression and macrophage infiltration in the kidney. EGb761 treatment at 48 hour before brain death significantly attenuate the levels of p-JNK-MAPK, p-p38-MAPK, and p-STAT3 proteins (all P < 0.05, compared to BD group). In summary, our data showed that EGb761 treatment protected donor kidney from BD-induced damages by blocking SAPK and JAK-STAT signalings. Early administration of EGb761 can provide better protective efficacy.
International Journal of Clinical Practice | 2015
L. Liu; Jun Li; X.-T. Chen; Huanxi Zhang; Qing-Ling Fu; Hui Yun Wang; Y.-Y. Xiong; Siyang Liu; Xiaoping Liu; Jia Li Li; Ma Yan Huang; C. Wang
To assess the efficacy and safety of tacrolimus and cyclosporin A (CsA)‐based immunosuppressive regimens in Chinese de novo kidney transplant recipients who are CYP3A5 expressers.
International Journal of Clinical Practice | 2016
Huanxi Zhang; L. Liu; Jia Li Li; Qing-Ling Fu; J. Wan; R. Deng; Hui Yun Wang; J. Liao; W. Deng; S. Deng; Lianzhou Chen; C. Wang
The aim of this study was to investigate the efficacy and safety of a transient intensified enteric‐coated mycophenolate sodium (EC‐MPS) dosing regimen with low exposure of calcineurin inhibitors (CNIs) in Chinese de novo kidney transplantation.
Transplantation Proceedings | 2018
L. Liu; Bin Ren; Huanxi Zhang; Jun Li; Qian Fu; Jiajia Jiang; S. Deng; Jiang Qiu; G. Chen; J. Fei; Lizhong Chen; C. Wang
BACKGROUND We calculated the population pharmacokinetics of mizoribine in adult Chinese patients and compared the parameters with those of Japanese patients to determine whether there are any ethnic differences in blood concentration transition between these 2 populations. METHODS The blood concentrations of mizoribine in 21 Chinese patients who were administered mizoribine after renal transplantation were measured at 304 time points. The absorption lag time, absorption rate constant, apparent distribution volume, and oral clearance were thereafter calculated and compared with the respective Japanese references. RESULTS The absorption lag time, absorption rate constant, and apparent distribution volume calculated in this study were, respectively, 0.353 hour, 0.856 hour-1, and 0.776 L/kg. The oral clearance was calculated as 2.18 times the creatinine clearance using creatinine clearance as a function. The absorption rate constant, apparent distribution volume, and oral clearance are determinants of the maximum blood concentration, trough, and area under the blood concentration time curve. The relative absorption rate constant, apparent distribution volume, and oral clearance were 0.9-, 0.9-, and 1.2-fold, respectively, in Chinese patients compared with those in Japanese patients. These values are within the confidence limit, suggesting that there is no significant PK difference between the 2 ethnic groups. CONCLUSIONS Results of this study showed no ethnic difference in blood mizoribine concentration transition between Chinese and Japanese patients. In addition, the population pharmacokinetic parameters obtained in this study are useful in determining the initial dosage or in the Bayesian analysis of mizoribine concentrations using scarce time points.
Transplantation | 2018
Huanxi Zhang; L. Liu; Jinqi Liu; Weijian Nie; Qian Fu; Ronghai Deng; Jun Li; C. Wang
Objective To investigate the risk factors of prolonged recovery from delayed graft function (DGF) after deceased kidney transplantation and to evaluate the effect of prolonged recovery on the outcome. Methods We retrospectively analyzed 91 recipients with DGF after deceased kidney transplantation from 2007 to 2016 in our center. DGF recovery time is defined as the time required to achieve stable serum creatinine level. Recipients with DGF recovery time ≥ the median were assigned to the prolonged recovery group while the rest to the rapid recovery group. Result Ninety-one recipients with regular follow-up until graft function recovery were further divided into fast and prolonged recovery group. The median recovery time was 27 days (Interquartile range: 15-45 days). Donor terminal glomerular filtration rate (GFR) was significantly lower in the prolonged recovery group (N = 46) compared with the rapid recovery group (N = 45) (median 24.9 vs 65.4 ml/min/1.73m2, P=0.0036). There was a significant decrease in the GFR at 1 year post-transplant in the prolonged recovery group compared with the rapid recovery group (50.6±20.0 vs 63.5±21.4 ml/min/1.73m2, P =0.005). The prolonged recovery group was also at higher risk of composite end-point (acute rejection, pneumonia, graft failure and death; hazards ratio 2.604, 95% confidence interval 1.102-6.150, P=0.029) compared with the rapid recovery group. Conclusion Donor acute kidney injury is a risk factor of prolonged recovery from DGF after deceased kidney transplantation. Prolonged recovery time is associated with restricted recovery of graft function and poor transplant outcome.
Pediatric Transplantation | 2018
Huanxi Zhang; Jiayue Luo; L. Liu; Jun Li; Qian Fu; Wenfang Chen; Shicong Yang; Wenjun Shang; Hong-yang Wang; Ronghai Deng; Liangzhong Sun; Xiaofeng Zhu; C. Wang
The choice of KT only or CLKT for infantile NPHP with mild liver fibrosis is understudied. A 5‐year‐old girl was transferred to our center for KT due to ESRD. Her primary disease was infantile NPHP with compound heterozygous NPHP3 mutations: c.458A>C(p.Q153P)/missense mutation and c.2032A>T(p. K678X)/nonsense mutation. The patient had elevated liver enzymes and biopsy‐proven liver fibrosis. As liver synthesis was acceptable, only KT was performed. However, liver fibrosis progressed at 1.5 years after transplantation, manifested with portal hypertension and hypersplenism. Common causes for portal hypertension were excluded, and the progression was attributed to NPHP. AMR attacked allograft at about 2 years post‐transplant. To solve both the liver and the kidney problems, CLKT was performed. Her liver and kidney function recovered initially, but she unfortunately died of pneumonia and subsequent intracranial hemorrhage two weeks later. Nonsense mutation in NPHP3 gene may be correlated with rapid progression of liver disease in infantile NPHP. More studies are required to determine the role of CLKT in these cases; however, combined transplantation may improve long‐term graft and patient survival.
Oncotarget | 2018
Huanxi Zhang; Linli Zheng; Shuhang Qin; L. Liu; Xiaopeng Yuan; Qian Fu; Jun Li; Ronghai Deng; S. Deng; Fangchao Yu; Xiaoshun He; C. Wang
Background This study aimed to evaluate the predictive power of five available delayed graft function (DGF)-prediction models for kidney transplants in the Chinese population. Results Among the five models, the Irish 2010 model scored the best in performance for the Chinese population. Irish 2010 model had an area under the receiver operating characteristic (ROC) curve of 0.737. Hosmer-Lemeshow goodness-of-fit test showed that the Irish 2010 model had a strong correlation between the calculated DGF risk and the observed DGF incidence (p = 0.887). When Irish 2010 model was used in the clinic, the optimal upper cut-off was set to 0.5 with the best positive likelihood ratio, while the lower cut-off was set to 0.1 with the best negative likelihood ratio. In the subgroup of donor aged ≤ 5, the observed DGF incidence was significantly higher than the calculated DGF risk by Irish 2010 model (27% vs. 9%). Materials and Methods A total of 711 renal transplant cases using deceased donors from China Donation after Citizens Death Program at our center between February 2007 and August 2016 were included in the analysis using the five predictive models (Irish 2010, Irish 2003, Chaphal 2014, Zaza 2015, Jeldres 2009). Conclusions Irish 2010 model has the best predictive power for DGF risk in Chinese population among the five models. However, it may not be suitable for allograft recipients whose donor aged ≤ 5-year-old.
Chinese Medical Journal | 2017
Hong-yang Wang; L. Liu; Hai-Ming Cao; Jun Li; Ronghai Deng; Qian Fu; Huanxi Zhang; J. Fei; C. Wang
Background: Accumulating studies on computational fluid dynamics (CFD) support the involvement of hemodynamic factors in artery stenosis. Based on a patient-specific CFD model, the present study aimed to investigate the hemodynamic characteristics of transplant renal artery stenosis (TRAS) and its alteration after stent treatment. Methods: Computed tomography angiography (CTA) data of kidney transplant recipients in a single transplant center from April 2013 to November 2014 were reviewed. The three-dimensional geometry of transplant renal artery (TRA) was reconstructed from the qualified CTA images and categorized into three groups: the normal, stenotic, and stented groups. Hemodynamic parameters including pressure distribution, velocity, wall shear stress (WSS), and mass flow rate (MFR) were extracted. The data of hemodynamic parameters were expressed as median (interquartile range), and Mann–Whitney U-test was used for analysis. Results: Totally, 6 normal, 12 stenotic, and 6 stented TRAs were included in the analysis. TRAS presented nonuniform pressure distribution, adverse pressure gradient across stenosis throat, flow vortex, and a separation zone at downstream stenosis. Stenotic arteries had higher maximal velocity and maximal WSS (2.94 [2.14, 3.30] vs. 1.06 [0.89, 1.15] m/s, 256.5 [149.8, 349.4] vs. 41.7 [37.8, 45.3] Pa at end diastole, P = 0.001; 3.25 [2.67, 3.56] vs. 1.65 [1.18, 1.72] m/s, 281.3 [184.3, 364.7] vs. 65.8 [61.2, 71.9] Pa at peak systole, P = 0.001) and lower minimal WSS and MFRs (0.07 [0.03, 0.13] vs. 0.52 [0.45, 0.67] Pa, 1.5 [1.0, 3.0] vs. 11.0 [8.0, 11.3] g/s at end diastole, P = 0.001; 0.08 [0.03, 0.19] vs. 0.70 [0.60, 0.81] Pa, 2.0 [1.3, 3.3] vs. 16.5 [13.0, 20.3] g/s at peak systole, P = 0.001) as compared to normal arteries. Stent implantation ameliorated all the alterations of the above hemodynamic factors except low WSS. Conclusions: Hemodynamic factors were significantly changed in severe TRAS. Stent implantation can restore or ameliorate deleterious change of hemodynamic factors except low WSS at stent regions.