Evaluation of G3BP1 in the prognosis of acute and acute-on-chronic liver failure after the treatment of artificial liver support system

Table 1 Clinical parameter baseline data for training cohort, validation cohorts and prospective confirmatory cohorts

Variable1	DifG3BP1 in training cohort					Validation cohorts
	Overall	T1 (< 0)	T2 (0-1)	T3 (> 1)	P value2
Patients (n)	244	83	120	41		514
Age (yr), mean ± SD	51.9 ± 13.2	53.20 ± 12.08	50.91 ± 14.07	52.10 ± 13.10	0.477	54.35 ± 15.6
Men, n (%)	204 (83.6)	68 (81.9)	99 (82.5)	37 (90.2)	0.45	426 (82.8)
AFP, mean ± SD	108.93 ± 170.12	68.65 ± 119.17	124.85 ± 180.26	143.86 ± 211.32	0.024	106.94 ± 114.56
WBC, mean ± SD	7.19 ± 3.54	8.28 ± 4.26	6.61 ± 2.97	6.70 ± 3.00	0.002	7.43 ± 3.65
N%, mean ± SD	69.38 ± 11.85	72.79 ± 10.60	67.33 ± 12.39	68.50 ± 11.35	0.004	71.34 ± 12.38
SAA, mean ± SD	9.33 ± 14.10	10.27 ± 13.57	9.61 ± 15.09	6.63 ± 11.99	0.385	9.56 ± 13.87
CRP, mean ± SD	14.03 ± 20.31	17.94 ± 23.64	12.09 ± 17.93	11.78 ± 18.84	0.096	13.67 ± 18.48
PCT, mean ± SD	0.62 ± 0.75	0.76 ± 0.92	0.55 ± 0.68	0.56 ± 0.54	0.13	0.65 ± 0.71
ALB (g/L), mean ± SD	31.23 ± 4.00	30.99 ± 3.53	31.36 ± 4.43	31.31 ± 3.61	0.799	32.56 ± 4.15
PTA (%), mean ± SD	43.69 ± 20.01	37.24 ± 15.90	46.35 ± 21.99	48.97 ± 18.40	0.001	42.17 ± 21.03
PT, mean ± SD	20.56 ± 6.21	23.13 ± 7.09	19.41 ± 5.41	18.74 ± 4.85	< 0.001	19.15 ± 6.12
INR, mean ± SD	1.83 ± 0.59	2.07 ± 0.70	1.72 ± 0.48	1.67 ± 0.47	< 0.001	1.87 ± 0.61
ALT, mean ± SD	276.93 ± 546.24	185.54 ± 266.86	332.65 ± 701.28	298.85 ± 420.08	0.162	295.13 ± 537.87
TBIL, mean ± SD	322.21 ± 131.10	353.56 ± 150.78	303.54 ± 122.07	313.37 ± 101.51	0.024	317.81 ± 145.11
AST, mean ± SD	247.66 ± 468.92	179.95 ± 188.58	292.26 ± 623.86	254.20 ± 299.16	0.244	238.98 ± 464.17
LDH, mean ± SD	273.07 ± 82.84	302.18 ± 70.80	250.64 ± 84.55	279.78 ± 82.64	< 0.001	286.46 ± 86.78
GFR, mean ± SD	101.69 ± 25.05	97.36 ± 27.28	104.94 ± 24.51	100.96 ± 20.71	0.104	102.54 ± 26.33
PLT, mean ± SD	111.18 ± 67.19	96.40 ± 66.11	118.06 ± 64.91	120.95 ± 72.38	0.046	106.54 ± 71.77
Family history of liver disease, n (%)3	36 (14.75)	14 (16.9)	17 (14.2)	5 (12.2)	0.763	78 (15.2)
Treatment method = PE + DPMAS (%)	20 (8.20)	7 (8.6)	6 (7.3)	7 (8.6)	0.938	46 (8.9)
LOS time (months), mean ± SD	35.55 (20.63)	34.36 (19.78)	36.51 (22.33)	35.75 (19.84)	0.797	35.78 (21.34)
Diabetes, n (%)	33 (13.52)	11 (13.6)	8 (9.8)	14 (17.3)	0.373	69
ALF, n (%)	53 (21.72)	14 (26.41)	29 (54.72)	10 (18.87)		111 (21.60)
ACLF, n (%)	191 (78.28)	69 (36.13)	91 (47.64)	31 (16.23)		403 (78.40)

¹Continuous variables are expressed as mean ± SD or median, categorical variables are expressed as n (%).

²Comparing the covariates across the 3 categories of the difference of G3BP1 between the level of discharge and admission.

³The family history included hepatitis B, liver cirrhosis, and liver cancer.

ACLF: Acute-on-chronic liver failure; AFP: Alpha-fetoprotein; ALB: Albumin; ALF: Acute liver failure; ALT: Alanine aminotransferase; AST: Aspartate transaminase; CRP: C-reactive protein; DifG3BP1: Difference of G3BP1 between the level of discharge and admission; DPMAS: Dual plasma molecular adsorption system; GFR: Glomeruar filtration rate; INR: International normalized ratio; LDH: Lactate dehydrogenase; N%: Neutrophil percent; PCT: Procalcitonin; PE: Plasma exchange; PLT: Platelet; PTA: Prothrombin activity; PT: Prothrombin time; SAA: Serum amyloid A protein; TBIL: Total bilirubin; WBC: White blood cell. T1 group: The group patients with the changed value of difference of G3BP1 between the level of discharge and admission discharge and admission (difG3BP1) was less than 0; T2 group: The group patients with the changed value of difG3BP1 was more than 0 and less than 1; T3 group: The group patients with the changed value of difG3BP1 was more than 1.

Table 2 Multivariable Cox regression analyses of difference of G3BP1 between the level of discharge and admission discharge and admission for predicting the risk for progression in training cohort

	G3BP1 cut points	Progression (%)1	Unadjusted HR (95%CI)	P value	Model 13	Adjusted HR (95%CI) P value
Total cohort (n = 244)
T1 + T2 G3BP1 (n = 161)	≥ 0	14 (8.7)	1.0 (Reference)		1.0 (Reference)
T3 G3BP1 (n = 83)	< 0	64 (77.1)	11.70 (6.50-21.04)	< 0.001	9.23 (5.08-16.75)	< 0.001
Subgroup with MELD2 high risk (n = 154)
T2 + T3 G3BP1 (n = 94)	≥ 0	13 (13.8)	1.0 (Reference)		1.0 (Reference)
T1 G3BP1 (n = 60)	< 0	53 (88.3)	8.01 (4.33-14.81)	< 0.001	5.71 (3.04-10.74)	< 0.001
Subgroup with MELD low-medium risk (n = 90)
T2 + T3 G3BP1 (n = 67)	≥ 0	1 (1.5)	1.0 (Reference)		1.0 (Reference)
T1 G3BP1 (n = 23)	< 0	11 (47.8)	39.46 (5.05-308.3)	< 0.001	23.80 (2.96-191.3)	< 0.001

¹The progression was death or liver transplantation.

²Model for end-stage liver disease score = 3.78 × ln [total bilirubin (μmol/L)/17.1] + 11.2 × ln (international normalized ratio) + 9.57 × ln [creatinine (μmol/L)/88.4] + 6.43. The higher the score, the worse the prognosis. The score of low risk is ≤ 14 points, the score of medium risk is 15-18 points, and the score of high risk is > 18 points.

³Model 1 adjusts the linear variables lactate dehydrogenase, alpha-fetoprotein.

HR: Hazard ratio; MELD: Model for end-stage liver disease.

Table 3 Multivariable Cox regression analyses of biomarkers for predicting the risk for progression in training cohort

Biomarker	G3BP1 cut points	Progression (%)	Unadjusted HR (95%CI)	P value	Model 11	Adjusted HR (95%CI) P value
IL-1β (pg/mL)
T1 IL-1β (n = 122)	≤ 168.0	15 (12.3)	1.0 (Reference)		1.0 (Reference)
T2 IL-1β (n = 122)	> 168.0	58 (47.5)	5.38 (3.03-9.54)	< 0.01	4.27 (2.37-7.67)	< 0.01
IL-18 (pg/mL)
T1 IL-18 (n = 122)	≤ 13.425	38 (31.1)	1.0 (Reference)		1.0 (Reference)
T2 IL-18 (n = 122)	> 13.425	35 (28.7)	0.94 (0.59-1.49)	0.78	0.95 (0.59-1.52)	0.83
TNF-α (pg/mL)
T1 TNF-α (n = 122)	≤ 5.465	46 (37.7)	1.0 (Reference)		1.0 (Reference)
T2 TNF-α (n = 122)	> 5.465	27 (22.1)	0.50 (0.31-0.80)	< 0.01	0.55 (0.34-0.90)	0.02

¹Model 1 adjusts the linear variables lactate dehydrogenase, alpha-fetoprotein.

HR: Hazard ratio; IL: Interlenkin; TNF-α: Tumor necrosis factor-α.

Table 4 Performance of biomarkers and/or clinical data for predicting risk for progression in training and validation cohorts

Biomarkers	C statistic (95%CI)1
	Training cohort (n = 244)	Validation cohort (n = 514)2
Univariable models of biomarkers
G3BP1	0.75 (0.68-0.81)	0.75 (0.71-0.78)
IL-1β	0.68 (0.63-0.74)
IL-18	0.54 (0.48-0.63)
TNF-α	0.57 (0.50-0.64)
Clinical models
Clinical data	0.78 (0.72-0.84)	0.71 (0.66-0.76)
Models containing clinical data and biomarkers
Clinical data + G3BP1	0.84 (0.77-0.89)	0.80 (0.76-0.84)
Clinical data + IL-1β	0.80 (0.75-0.85)
Clinical data + IL-18	0.78 (0.72-0.84)
Clinical data + TNF-α	0.78 (0.72-0.84)
Model containing clinical data and multiple biomarkers
Clinical data + G3BP1 + IL-1β + IL-18 + TNF-α3	0.84 (0.79-0.90)

¹Expressed as Harrell’s C-index, continuous biomarkers were used in the model.

²Due to limited sample availability of the validation cohort, only G3BP1 assay was performed for participants from the cohort.

³Comprising lactate dehydrogenase, alpha-fetoprotein.

HR: Hazard ratio; IL: Interlenkin; TNF-α: Tumor necrosis factor-α.