Gamma-glutamyl transpeptidase and indirect bilirubin may participate in systemic inflammation of patients with psoriatic arthritis

Wang, Xu; Mao, Yan; Ji, Shang; Hu, Huanrong; Li, Qian; Liu, Lichao; Shi, Shaomin; Liu, Yaling

doi:10.1186/s42358-023-00334-y

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Sumário

Research • Adv. rheumatol. 63 • 2023 • https://doi.org/10.1186/s42358-023-00334-y copy

Gamma-glutamyl transpeptidase and indirect bilirubin may participate in systemic inflammation of patients with psoriatic arthritis

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Background

Previous studies have suggested that systemic metabolic abnormalities are closely related to psoriatic arthritis (PsA). Gamma-glutamyl transpeptidase (GGT) and indirect bilirubin (IBIL), two essential active substances in hepatic metabolism that have been demonstrated as an oxidative and anti-oxidative factor respectively, have been proved to be involved in oxidative stress damage and inflammation in several human diseases. However, their role in PsA remains unclear.

Methods

In this retrospective comparative cohort study, a case group of 68 PsA patients and a control group of 73 healthy volunteers from the Third Hospital of Hebei Medical University were enrolled. Serum GGT, IBIL, GGT/IBIL ratio and C-reactive protein (CRP), a well applied bio-marker of systemic inflammatory in PsA, were compared between the two groups. Furthermore, the relationship of GGT, IBIL and GGT/IBIL with CRP were explored in PsA patients. Finally, the patients were divided into high inflammation group and low inflammation group according to the median value of CRP. Multivariate logistic regression analyses were used for the association of systemic inflammation level with GGT, IBIL and GGT/IBIL.

Results

Compared with healthy controls, PsA patients exhibited significantly higher serum GGT, GGT/IBIL, and CRP levels and lower IBIL levels. Serum GGT and GGT/IBIL were positively correlated with CRP, whereas IBIL were negatively correlated with CRP. Binary logistic regression analysis revealed that serum GGT was a risk factor for high CRP in PsA, whereas IBIL was a protective factor. Furthermore, GGT/IBIL was a better indicator of high CRP condition in PsA patients than either GGT or IBIL alone, as determined by the receiver operating characteristic curves.

Conclusion

GGT and IBIL may participate in the pathogenesis of PsA. Additionally, GGT, IBIL and the balance of the two may reflect systemic inflammation mediated by oxidative stress events related to metabolic abnormalities to a certain extent.

Keywords
Psoriatic arthritis; Gamma-glutamyl transpeptidase; Indirect bilirubin; C-reactive protein; Inflammation

	PsA patients (n = 68)	Controls (n = 73)	P
Gender (male/female)	44/24	38/35	0.128
Age (years)	44.5 (33.0, 54.8)	44.0 (35.0, 51.0)	0.836
CRP (mg/L)	20.8 (6.9, 60.5)	1.5 (1.2, 2.8)	< 0.001
ALT (U/L)	15.5 (11.0, 25.8)	18.0 (12.0, 27.5)	0.068
AST (U/L)	15.0 (14.0, 19.8)	17.0 (15.0, 20.0)	0.111
GGT (U/L)	24.0 (16.3, 36.8)	19.0 (15.0, 30.5)	0.036
IBIL (μmol/L)	6.9 (4.4, 9.3)	10.1 (8.2, 11.9)	< 0.001
GGT/IBIL ratio	3.8 (2.1, 8.3)	2.0 (1.5, 2.9)	< 0.001

	PsA1	PsA2	P
Gender (male/female)	16/18	22/12	0.143
Age (years)	49.0 (34.0, 55.5)	41.5 (32.8, 54.3)	0.286
ALT (U/L)	14.0 (11.0, 19.0)	16.5 (10.0, 27.5)	0.400
AST (U/L)	15.5 (14.0, 18.3)	15.0 (13.0, 20.3)	0.956
GGT (U/L)	22.5 (15.0, 27.0)	33.5 (20.0, 71.5)	0.002
IBIL (μmol/L)	8.7 (5.5, 12.5)	6.1 (3.9, 7.3)	0.003
GGT/IBIL ratio	2.2 (1.5, 4.3)	7.0 (3.1, 14.7)	< 0.001

Parameters	B	SE	Wald	OR	95% CI	P
Gender	−0.998	0.664	2.258	0.369	0.100–1.355	0.133
Age	−0.017	0.028	0.377	0.983	0.931–1.038	0.539
ALT	−0.011	0.052	0.047	0.989	0.892–1.095	0.828
AST	−0.065	0.066	0.996	0.937	0.824–1.065	0.318
GGT	0.071	0.033	4.574	1.073	1.006–1.145	0.032
IBIL	−0.266	0.098	7.411	0.766	0.633–0.928	0.006
Constant	2.342	1.751	1.790	10.402	–	0.181

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[1] *Correspondence: Shaomin Shi dermatologist_shi@163.com Yaling Liu yzling_liu1214@126.com