Erythrocyte count is associated with prognosis in Chinese patients with primary biliary cholangitis.

Erythroid parameters have been indicated to be important prognostic factors for liver diseases. The present study aimed to evaluate the prognostic value of the erythrocyte count in Chinese patients with primary biliary cholangitis (PBC) and develop a prognostic model. The clinical data of 301 patients with PBC were retrospectively reviewed. Univariate and multivariate Cox regression analysis was performed to identify potential prognostic risk factors. Bivariate correlation analysis was used to determine the correlation coefficient of the erythrocyte count and biochemical indices. The prognostic values of different factors were compared by receiver operating characteristic (ROC) curve analysis. A novel prognostic model was constructed using multivariate logistic regression. Multivariate regression analysis suggested that the erythrocyte count was an independent risk factor/prognostic index (P=0.042). The erythrocyte count in peripheral blood decreased as the histological stage progressed (P<0.001). The erythrocyte count was correlated with albumin, liver stiffness and Fibrosis-4. Compared with that of platelets, the area under the ROC curve of the erythrocyte count was significantly greater. A similar area under the ROC curve was determined for the erythrocyte count, albumin and total bilirubin (P>0.05). A novel prognostic model was established as follows: P=1/{1 + e-[6.140-3.193 × Ln(erythrocyte count) -0.184 × albumin + 0.827 × Ln(total bilirubin)]}. The novel model had a comparable prognostic value to that of the GLOBE score and UK-PBC risk score, and had a better performance than the Mayo risk score at baseline (0.838 vs. 0.787). In conclusion, the erythrocyte count is an independent risk factor/prognostic index in Chinese patients with PBC. It was correlated with liver function and fibrosis in Chinese patients. The novel model incorporating the erythrocyte count and biochemical indices at baseline may serve as a prognostic tool in Chinese patients with PBC (Trial registration number, ChiCTR-ONRC-10002070; date of registration, 2010-05-10). Copyright: © Chang et al.

Introduction

Primary biliary cholangitis (PBC) is a chronic and progressive immune-mediated cholestatic liver disease (1). The survival periods of patients with PBC vary. For patients diagnosed at the early stage, the survival periods are similar to those of healthy individuals after ursodeoxycholic acid (UDCA) treatment (2). The median survival time is 6–10 years for patients with advanced PBC (3). According to clinical practice guidelines, risk stratification has a vital role in the clinical management of patients with PBC (4). For risk stratification of patients with PBC, it is required to assess the probability of adverse events and perform a prediction of the prognosis prior to treatment. In order to predict the survival of patients with PBC, several prognostic models based on clinical parameters have been developed, including the GLOBE score, UK-PBC risk score and Mayo risk score (5–8).

All of the continuous scoring systems mentioned above have been widely used for prognostic evaluation in patients with PBC. Furthermore, several studies were performed to explore novel prognostic indices or models (5,7). Their results suggested that existing prognostic models of PBC may be improved by taking other variables into account. In previous years, erythroid-associated parameters have been indicated to be linked to liver-associated diseases (9,10). A previous study has reported that the erythrocyte count in peripheral blood was associated with survival after surgery in patients with primary liver cancer (11). Several other studies have reported that the red blood cell distribution width (RDW) may serve as a predictive index for histological severity and a potential prognostic indicator of chronic liver diseases (12–14). While the mechanism underlying the clinical relevance of erythrocytes in PBC remains elusive, previous studies have indicated that erythroid parameters, including the erythrocyte count, are potential prognostic indicators for PBC (12,13).

In the present study, the prognostic value of the erythrocyte count in Chinese patients with PBC was analyzed. Correlations of the erythrocyte count with liver-associated indices were investigated. Furthermore, a novel predictive model for the prognosis of PBC was developed by incorporating the erythrocyte count and other biochemical indices.

Patients and methods

Patients

The present study was approved by the Ethics Committee of Xijing Hospital (Xi'an, China) and all patients had signed an informed consent form. The present study was performed in accordance with the Declaration of Helsinki. The present study retrospectively enrolled 301 patients with PBC who received treatment at the Department of Gastroenterology at Xijing Hospital (Xi'an, China) from March 2006 to August 2018. Initiation of UDCA treatment was between March 2006 and January 2017. The inclusion criteria were as follows: i) Patients diagnosed with PBC meeting at least two of the following criteria: Alkaline phosphatase (ALP) >2-fold of the upper limit normal (ULN) or gamma-glutamyl transpeptidase (GGT) >5-fold of the ULN, titer of anti-mitochondrial antibody >1:40 and liver biopsy exhibiting florid bile duct lesions; ii) UDCA treatment was initiated and maintained for at least 12 months at the dosage of 13–15 mg/kg/day after diagnosis of PBC. The exclusion criteria were as follows: i) Concurrence of other liver diseases, including viral hepatitis, primary sclerosing cholangitis, autoimmune hepatitis, alcoholic liver disease, hemochromatosis, Wilsons disease or non-alcoholic steatohepatitis; ii) baseline clinical data were incomplete; iii) for patients with transplant-free survival, the duration of follow-up was <1 year. All patients had been followed up at intervals of 1–6 months during UDCA treatment. The ULN of ALP was 150 U/l and the ULN of GGT was 50 U/l.

Study design

Clinical data were retrieved from the patients' records at baseline and after 1 year of treatment. The data included the erythrocyte count, haemoglobin (HGB), hematocrit (HCT), erythrocyte mean corpuscular volume (MCV), age, sex, platelets (PLT), alanine aminotransferase (ALT), aspartate aminotransferase (AST), albumin (ALB), globulin (GLB), total bilirubin (TBIL), ALP, GGT, cholesterol, triglyceride (TG), creatinine (CRE), prothrombin time (PT), activated partial thromboplastin time (APTT), fibrinogen and thrombin time. Other demographic indices, including body mass index and status of smoking and drinking, were not included in the analysis, as they were not available. The GLOBE score and UK-PBC risk score were calculated after 1 year of treatment and the Mayo risk score was determined at baseline. Liver stiffness (LS) (15) and Fibrosis-4 (FIB-4) (16) were recorded at baseline and taken as indicators of liver fibrosis. LS was detected by transient elastography with FibroTouch (Wuxi Hisky Medical Technology Co., Ltd.). According to the formula in the Formulae of predictive models section below, the FIB-4 score was determined from four baseline variables, including age, AST, ALT and PLT. Pathological stages were classified according to Ludwig's classification (17) and presented as categorical data. The end-points were defined as liver transplantation or death.

Histological analysis

Liver biopsies were analyzed by two experienced hepatic pathologists (Professor Zengshan Li and Dr Lin Chen, Department of Pathology, Xijing Hospital, Fourth Military Medical University). Histological features were recorded as stage 1 (portal stage), stage 2 (periportal stage), stage 3 (septal stage) and stage 4 (cirrhosis) (17,18), according to Ludwig's classification.

Statistical analysis

Continuous variables with a normal distribution are expressed as the mean ± standard deviation, while variables with a non-normal distribution are presented as the median (lower quartile-upper quartile). Shapiro-Wilk test was applied to assess normality of distribution. Categorical variables were expressed as n (%). For comparison of categorical data, Fisher's exact test was performed. The Kruskal-Wallis H-test and Mann-Whitney U-test with Bonferroni correction were used for continuous values with a non-normal distribution. Hazard ratios (HRs) and 95% CIs of biochemical parameters were calculated using the Cox regression model in univariate and multivariate analyses. Bivariate correlation analysis was applied to determine correlations between erythrocyte count and liver-associated parameters and Spearman correlation coefficients were obtained. Receiver operating characteristic (ROC) curve analysis was utilized for evaluating the prognostic value of biochemical parameters and predictive models. Comparisons of areas under receiver operating characteristic curve (AUCs) of biochemical parameters and predictive models were accomplished by the Delong-Delong non-parametric method. Based on binary multivariate logistic regression analysis, a predictive model was constructed for estimating the prognosis at baseline. The Hosmer-Lemeshow test was applied to test for the goodness of fit of the predictive model. Analyses were accomplished using SPSS 19.0 (IBM Corp.), except for the comparisons of AUCs, which were performed with MedCalc Statistical Software version 15.2.2 (MedCalc Software bvba). The P-values were two-sided and P<0.05 was considered to indicate a statistically significant difference.

Formulae of predictive models

i) GLOBE score=0.044378 × age (years) at baseline + 0.93982 × ln(TBIL times ULN at one-year follow-up) + 0.335648 × ln(ALP times the ULN at one-year follow-up) −2.266708 × ALB times the lower limit of normal (LLN) at one-year follow-up −0.002581 × PLT count per 109/l at one-year follow-up + 1.216865 (6).

ii) UK-PBC risk score=1-0.9820.0287854 × (ALP at one-year follow-up/ULN-1.722136304) −0.0422873 × {[1/(AST at one-year follow-up/ULN/10)] −8.675729006} + 1.4199 × [ln(TBIL at one-year follow-up/ULN/10) + 2.709607778]-1.960303 × (ALB/LLN-1.17673001) −0.4161954 × (PLT/LLN-1.873564875) (7).

iii) FIB-4=[age (years) × AST (U/l)]/[PLT (109/l) × ] (16).

iv) Mayo risk score=0.039 × age (years) + 0.871 × ln[serum bilirubin (mg/dl)] −2.53 × ln[albumin (mg/dl)] + 2.38 × ln[prothrombin time (sec)] + 0.859 × ascites; (ascites: no=0, yes=1) (8).

Results

Patient characteristics

The demographic and clinical data of the present cohort are provided in Table I. A total of 301 Chinese patients with PBC were retrospectively reviewed, including 258 (85.7%) females and 43 (14.3%) males. The average age of the patients at baseline was 51.89 years. The median follow-up time was 44 months. Furthermore, 41 patients (13.6%) underwent liver transplantation or died during the follow-up.

Table I.

Features at baseline and after one year of therapy.

Parameter	Normal limit	Baseline	After one year of therapy	P-value
Erythrocytes (1012/l)	>4.00	3.94 (3.52–4.29)	4.24 (3.88–4.56)	<0.001
HGB (g/l)	>120.00	119.00 (105.00–131.00)	127.00 (111.00–137.00)	<0.001
HCT (%)	>40.0	36.7 (32.5–39.5)	38.9 (34.8–41.5)	<0.001
MCV (fl)	>80.00	93.00 (89.80–96.20)	92.40 (87.98–95.78)	0.064
PLT (109/l)	>100.00	137.00 (83.00–202.00)	146.00 (84.50–210.00)	0.304
ALT (U/l)	<40.00	58.00 (37.00–94.00)	33.00 (23.00–55.75)	<0.001
AST (U/l)	<40.00	63.00 (43.00–96.00)	38.00 (29.00–59.75)	<0.001
ALB (g/l)	>35.00	39.20 (36.00–41.80)	43.00 (39.90–45.50)	<0.001
GLB (g/l)	<32.00	30.75 (28.00–34.40)	31.80 (28.50–35.10)	0.178
TBIL (µmol/l)	<17.10	19.00 (12.70–32.00)	14.50 (10.83–21.40)	<0.001
ALP (U/l)	<150.00	263.00 (161.00–427.50)	162.50 (111.00–243.25)	<0.001
GGT (U/l)	<50.00	268.00 (118.50–425.00)	101.50 (42.00–211.50)	<0.001
CHO (mmol/l)	<5.18	4.43 (3.65–5.71)	4.85 (3.92–5.60)	0.090
TG (mmol/l)	<1.70	1.17 (0.77–1.69)	1.25 (0.92–1.84)	0.006
CRE (µmol/l)	<133.00	75.00 (66.00–84.00)	80.00 (72.00–88.50)	<0.001
PT (sec)	<13.00	12.90 (12.20–13.90)	12.90 (12.30–13.70)	0.929
APTT (sec)	<37.00	39.85 (36.20–43.73)	38.75 (35.48–42.58)	0.161
Fibrinogen (g/l)	>2.00	2.96 (2.50–3.52)	3.00 (2.51–3.54)	0.862
TT (sec)	<16.00	17.20 (16.40–18.00)	17.10 (16.30–18.40)	0.571
Age (years)		51.89±9.98
Female sex (%)		258 (85.7%)
Follow-up time[a] (months)		44 (27–60)
Stage (1/2/3/4)		22/119/48/65
Transplant-free survival[b] (%)		260 (86.4%)
LS (kPa)		9.91 (6.82–19.56)
FIB-4		3.287 (1.836–6.383)
Mayo risk score		4.847 (4.251–5.708)
GLOBE score			0.191 (−0.468–1.053)
UK-PBC risk score			0.0306 (0.0153–0.0726)

Duration from diagnosis to the end of follow-up or reaching the clinical end-point.

Survival without liver-associated death or liver transplantation. Continuous data are presented as the mean ± standard deviation or as the median with interquartile range and categorical data are expressed as the number with percentage. HGB, haemoglobin; HCT, hematocrit; MCV, erythrocyte mean corpuscular volume; PLT, platelets; ALT, alanine aminotransferase; AST, aspartate aminotransferase; ALB, albumin; GLB, globulin; TBIL, total bilirubin; ALP, alkaline phosphatase; GGT, gamma-glutamyltranspeptidase; CHO, cholesterol; TG, triglyceride; CRE, creatinine; PT, prothrombin time; APTT, activated partial thromboplastin time; TT, thrombin time; LS, liver stiffness; FIB-4, Fibrosis-4.

Prognostic factors of survival by univariate and multivariate regression analysis

According to the univariate Cox regression analysis, the baseline erythrocyte count, MCV, HGB, HCT, age, PLT, AST, ALB, GLB, TBIL, CRE, PT and APTT were associated with patient survival. A multivariate analysis was then performed for each of these baseline factors. The results indicated that only the erythrocyte count (P=0.042, HR: 0.524, 95%CI: 0.281–0.976), ALB (P<0.001, HR: 0.844, 95%CI: 0.792–0.900) and TBIL (P<0.001, HR: 1.008, 95%CI: 1.005–1.012) at baseline were independent risk factors and associated with patient prognosis (Table II).

Table II.

Prognostic value of baseline parameters in Cox regression analysis.

	Univariate analysis			Multivariate analysis
Baseline parameter	P-value	Hazard ratio	95% CI	P-value	Hazard ratio	95% CI
Age	<0.001	1.059	1.021–1.099
Sex (female/male)	0.960	0.978	0.411–2.328
Erythrocyte	<0.001	0.246	0.166–0.365	0.042	0.524	0.281–0.976
HGB	<0.001	0.969	0.958–0.981
HCT	<0.001	0.001	0.000–0.001
MCV	0.304	1.008	0.993–1.022
PLT	0.007	0.994	0.989–0.998
ALT	0.725	0.999	0.994–1.004
AST	0.057	1.003	1.000–1.006
ALB	<0.001	0.819	0.782–0.858	<0.001	0.844	0.792–0.900
GLB	0.053	1.044	0.999–1.091
TBIL	<0.001	1.011	1.008–1.014	<0.001	1.008	1.005–1.012
ALP	0.410	1.000	0.999–1.002
GGT	0.341	0.999	0.998–1.001
CHO	0.776	0.978	0.838–1.141
TG	0.910	0.979	0.684–1.403
CRE	0.028	0.973	0.949–0.997
PT	<0.001	1.385	1.215–1.579
APTT	0.001	1.076	1.030–1.124
Fibrinogen	0.234	0.779	0.516–1.175
TT	0.973	0.999	0.953–1.047

HGB, haemoglobin; HCT, hematocrit; MCV, erythrocyte mean corpuscular volume; PLT, platelets; ALT, alanine aminotransferase; AST, aspartate aminotransferase; ALB, albumin; GLB, globulin; TBIL, total bilirubin; ALP, alkaline phosphatase; GGT, gamma-glutamyltranspeptidase; CHO, cholesterol; TG, triglyceride; CRE, creatinine; PT, prothrombin time; APTT, activated partial thromboplastin time; TT, thrombin time.

Correlation of erythrocyte count with biochemical and fibrosis indices

Bivariate correlation analysis was used for determining linear correlation coefficients between the erythrocyte count and other baseline biochemical indices (Table SI). Close correlations were identified between the erythrocyte count and other parameters, including the PLT, ALB and TBIL (P<0.001). A positive correlation of the erythrocyte count with ALB (r=0.555) and PLT (r=0.329) was determined, as well as a negative correlation with TBIL (r=−0.406). The correlations between the erythrocyte count and hepatic fibrosis parameters were investigated to verify whether the erythrocyte count in the peripheral blood was associated with the progression of PBC. The erythrocyte count decreased as the pathological stage increased (P<0.001; Fig. 1; Table SII). There was a negative correlation between the erythrocyte count and the pathological stage (r=−0.410, P<0.001; Fig. S1). Furthermore, a bivariate correlation analysis was performed, suggesting that the erythrocyte count was closely linearly correlated to LS (r=−0.581, P=0.003) and FIB-4 (r=−0.482, P<0.001), indicating that the erythrocyte count was associated with the progression of cirrhosis in Chinese patients with PBC (Fig. 2).

Figure 1.

Comparison of erythrocyte count between patients with different histological stages. *P<0.05, **P<0.01.

Figure 2.

Correlation between erythrocyte count and fibrosis indexes in scatter plots. (A) Correlation between erythrocyte count and liver stiffness. (B) Correlation between erythrocyte count and FIB-4. FIB-4, Fibrosis-4.

Predictive performance of erythroid parameters for patient prognosis

The prognostic value of various biochemical indices was determined using ROC curve analysis at baseline and at the one-year follow-up. At baseline, the erythrocyte count had a significantly higher AUC value than HGB (0.822 vs. 0.762, P<0.001), HCT (0.822 vs. 0.782, P=0.002) and PLT (0.822 vs. 0.654, P=0.003; Fig. 3A). After UDCA treatment for one year, the erythrocyte count still had a significantly higher AUC value than PLT (0.821 vs. 0.676, P=0.006; Fig. 3B; Table III). The AUC of the erythrocyte count was comparable to that of ALB and TBIL (P>0.05) at baseline and at the one-year follow-up (Table SIII).

Figure 3.

Receiver operating characteristic curves presenting the prognostic value of parameters at baseline and after one year of therapy. (A) Prognostic value of various baseline parameters. (B) Prognostic value of parameters after one year of therapy. HGB, haemoglobin; HCT, hematocrit; PLT, platelet; ALB, albumin; TBIL, total bilirubin.

Table III.

Prognostic value of parameters at baseline and after one year of therapy.

A, Baseline
			Asymptotic 95% confidence interval
Parameter	Area	P-value	Lower	Upper
Erythrocyte count	0.822	<0.001	0.738	0.906
HGB	0.762	<0.001	0.674	0.851
HCT	0.782	<0.001	0.693	0.870
PLT	0.654	0.002	0.563	0.744
ALB	0.849	<0.001	0.785	0.914
TBIL	0.765	<0.001	0.687	0.843
B, After one year of treatment
			Asymptotic 95% confidence interval
Parameter	Area	P-value	Lower	Upper
Erythrocyte count	0.821	<0.001	0.730	0.912
HGB	0.783	<0.001	0.687	0.879
HCT	0.807	<0.001	0.715	0.898
PLT	0.676	0.003	0.575	0.777
ALB	0.835	<0.001	0.743	0.927
TBIL	0.846	<0.001	0.772	0.921

HGB, haemoglobin; HCT, hematocrit; PLT, platelets; ALB, albumin; TBIL, total bilirubin.

Derivation of predictive model for prognosis

Multivariate logistic regression analysis was performed on potential prognostic risk factors to construct a predictive model. Only variables identified in the multivariate Cox regression were included in the model. Ln transformations were applied for erythrocyte count and TBIL. The predictive model was constructed as follows:

P=1/{1 + e−[6.140–3.193 × Ln(erythrocyte count) −0.184 × ALB + 0.827 × LnTBIL]}.

Regarding goodness of fit, the result of the Hosmer- Lemeshow test was P=0.454. Subsequently, the performance of the novel predictive model was compared using the GLOBE score, UK-PBC risk score and Mayo risk score. At baseline, the novel model had a greater AUC value than the Mayo risk score (0.838 vs. 0.787), while the novel model had a similar AUC value compared with the GLOBE score and the UK-PBC risk score (P>0.05; Fig. 4; Table IV; Table SIV). The sensitivity and specificity of the predictive model were 80.0 and 85.1% for predicting transplant-free survival according to the maximum Youden index.

Figure 4.

Receiver operating characteristic curves presenting the prognostic value of various predictive score systems.

Table IV.

Receiver operating characteristic parameters presenting the prognostic value of predictive score systems.

			Asymptotic 95% confidence interval
Scoring system	Area under curve	P-value	Lower	Upper	Sensitivity (%)	Specificity (%)
Predictive model (>0.16)	0.838	<0.001	0.747	0.929	80.0	85.1
Mayo risk score (>6.10)	0.787	<0.001	0.668	0.907	74.4	88.5
GLOBE score (>0.83)	0.893	<0.001	0.812	0.974	92.9	76.4
UK-PBC risk score (>0.092)	0.884	<0.001	0.809	0.959	78.6	87.2

Discussion

Abnormalities of peripheral blood erythroid parameters have been observed in several liver diseases. In recent years, certain studies with limited patients indicated a potential prognostic value of erythroid parameters in patients with PBC (12,13). The decrease in erythrocyte count may be attributed to several aspects. As a common reason for the decrease of the erythocyte count, hemolysis presents in up to 50% of patients with chronic liver disease regardless of etiologies (19). Complications of cirrhosis, including splenomegaly, are the major reasons for hemolysis in patients with end-stage disease. Alterations of the lipid composition, which were detected in the erythrocyte membrane of patients with liver diseases, have been associated with liver damage (20,21). The erythrocyte count in peripheral blood may be associated with chronic hepatic injury due to the impairment of the erythrocyte membrane structure caused by alteration of the lipid composition. Furthermore, certain studies suggested that the deficiency of hematopoietic precursors due to immune injury of the hematopoietic system was also linked to a reduced erythrocyte count in patients with PBC (22,23). Other causes of erythrocyte deficiency included malnutrition, iron deficiency, bone marrow depression, cirrhosis and medications (22,24).

Splenomegaly is a cause of decreased erythrocyte count in patients with end-stage PBC and it is considered to be linked to poor prognosis. However, in the present study, splenomegaly was not subjected to multivariate Cox regression analysis, as the results of the imaging examination at baseline were not available for all patients. The relevance of splenomegaly regarding the prognostic value of the erythrocyte count requires to be clarified. The mechanisms underlying the correlations between erythrocytes and liver fibrosis or dysfunction in patients with PBC also require to be further clarified. In the present study, a close correlation between erythrocyte count and liver function parameters, including ALB and TBIL, was identified. Furthermore, the erythrocyte count decreased as the pathological stage and liver fibrosis progressed. The increase in erythrocyte count after UDCA treatment was accompanied by the improvement of liver function and liver fibrosis score. Therefore, the decrease of the erythrocyte count may reflect the severity of liver disease and the extent of liver function deficiency in patients with PBC, which is in accordance with a previous study in patients with primary liver cancer (11).

Early prognostic models are important for risk stratification for patients with PBC. In the present study, the prognostic value of the erythrocyte count was investigated as a simple, routinely tested parameter in Chinese patients with PBC. The novel predictive model incorporating the erythrocyte count had a better prognostic performance than the Mayo risk score, one of the most widely used prognostic systems (25), and was comparable with the GLOBE score and UK-PBC risk score in the evaluation of the prognosis regarding transplant-free survival. The GLOBE score and UK-PBC risk score involve parameters after one year of UDCA treatment. The novel model included only parameters at baseline, which may be helpful for early prognosis evaluation prior to initiation of UDCA treatment.

The present study has certain limitations. First, the present study was a retrospective study performed in only one clinical center. More prospective studies are required to confirm the results of the present study. Furthermore, no validation of the novel model was performed in another PBC cohort. The present cohort was only comprised of Chinese patients with PBC from one hospital. Although the sample size of the cohort was relatively big, it is still required to validate the prognostic model in other cohorts in China and other populations. Furthermore, RDW has been reported to be of prognostic value in PBC patients. RDW data were missing from the clinical data of the present cohort, making it impossible to verify the results of previous studies and to determine whether RDW is a surrogate parameter for the erythrocyte count in the prognosis of PBC.

In conclusion, the present study indicated that the erythrocyte count is a useful prognostic parameter in Chinese patients with PBC. The peripheral blood erythrocyte count was closely correlated with liver dysfunction and fibrosis. The model incorporating the erythrocyte count, ALB and TBIL may serve as an early prognostic tool for PBC.