Endothelial cell injury with inflammatory cytokine and coagulation in patients with sepsis

doi:10.5847/wjem.j.issn.1920-8642.2013.04.008

Abstract

Abstract:

BACKGROUND: Current studies on CD62P have focused mainly on cardiovascular diseases, while only few studies have evaluated the effects of CD62P on the development of sepsis and the association between endothelial cell injury with inflammation and coagulation. This study attended to explore the association between endothelial cell injury with inflammation and coagulation by evaluating the expression of soluble CD62P (s-CD62P) in plasma and its mechanism in patients with sepsis, thus to provide the evidence of effective treatment of sepsis with anti-adhesion therapy targeted CD62P.
METHODS: A total of 70 critically ill patients with systemic inflammatory response syndrome (SIRS) admitted to intensive care unit (ICU) between September 2009 and February 2010 were enrolled for a prospective and control study. According to the diagnostic criteria of sepsis/SIRS, the patients were divided into two groups: a sepsis group (n=38) and a SIRS group (n=32). Another 20 healthy volunteers served as a control group. Patients in the sepsis group and SIRS group were matched by clinical signs of high blood pressure, diabetes and its complications. The demographics of the patients including age, sex, body mass index (BMI), smoking and alcohol addict were compared among the groups. Six mL peripheral blood samples were collected within 24-hour admission in ICU for enzyme-linked immunosorbent assay (ELISA) to detect the plasma levels of s-CD62P, TNF-α, and hs-CRP. And variables of coagulation function such as platelet (PLT), prothrombin (PT), activated partial thromboplastin time (APTT), D-dimer and antithrombin-III (AT-III) were analyzed during 24 hours after admission to ICU. Meanwhile sequential organ failure assessment (SOFA) score of critically ill patients was evaluated. Data were expressed as mean±standard deviation and were statistically analyzed by using SPSS 17.0 statistical software. The differences in plasma levels of s-CD62P of patients in each group were analyzedby ANOVA and the Kruskal-Wallis test. The relations between s-CD62P and inflammatory cytokines as well as with coagulation were determined by Pearson's product moment correlation coefficient analysis. Changes were considered as statistically significant if P value was less than 0.05.
RESULTS: Compared with the control group and SIRS group, the sepsis group demonstrated significantly higher levels of s-CD62P, TNF-α and highly sensitive C-reactive protein (hs-CRP) (P<0.05). The plasma levels of D-dimer, PT, and APTT in the sepsis and SIRS groups were significantly higher than those in the control group, while the platelet count and the activity of AT-III were obviously lower (P<0.05). In the sepsis group, the plasma levels of hs-CRP and TNF-α were positively correlated with PT, APTT, and D-dimer, and negatively correlated with AT-III and PLT (P<0.05). The plasma levels of s-CD62P were significantly correlated with the plasma levels of TNF-α, hs-CRP, D-dimer, PT, and APTT, whereas they were correlated negatively well with PLT and AT-III (P<0.05).
CONCLUSIONS: The concentration of plasma s-CD62P is elevated as a early biomarker in patients with sepsis, and it serves as one of the pathogenic factors responsible for endothelial cell damage. Coagulation and mediators of inflammation promote each other, aggravating the severity of sepsis. Plasma s-CD62P may be an important factor for the development of coagulation and inflammatory reaction.

Key words: Sepsis, Endothelial cell injury, Plasma soluble CD62P, Inflammatory cytokine, Coagulation

Huan Ding, Xiang-yuan Cao, Xi-gang Ma, Wen-jie Zhou. Endothelial cell injury with inflammatory cytokine and coagulation in patients with sepsis[J]. World Journal of Emergency Medicine, 2013, 4(4): 285-289.

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Variables	Sepsis group (n=38)	SIRS group (n=32)	Control group (n=20)	F value or χ²value	P value
Age (year, x±s)	56.4±18.70	49.22±22.99	48.9±10.06	1.058	0.354
Male/female	29/9	25/7	16/4	0.807	0.668
BMI (x±s)	23.31±3.72	23.69±3.54	23.73±3.13	0.136	0.873
Smoker	18	12	5	2.799	0.247
Drinker	12	9	8	0.807	0.668
Comorbity
Hypertension	7	6	_	0.972	1.000
Diabetes	5	6	_	0.410	0.522
Diabetes and its complications	26	24	_	0.368	0.544
SOFA score (x±s)	7.33±3.11	5.44±2.89		16.134	0.000

Groups	s-CD62P (ng/mL)	hs-CRP (mg/L)	TNF-α (pg/mL)
Sepsis group (n=38)	221.74±77.09^*#	91.53±55.81^*#	32.28±14.98^*#
SIRS group (n=32)	119.64±52.96	18.48±12.32	15.43±6.39^*
Control group (n=20)	97.71±35.90	3.28±1.91	5.29±1.78
F value or tvalue	21.142	26.832	25.715
P value	0.000	0.000	0.000

Groups	Platelet count	PT (s)	APTT (s)	D-dimer (μg/L)	AT-III (%)
Sepsis group (n=38)	152.59±115.34^*	13.48±2.18^*	37.47±14.65^*	726.00 (163-2 765)^*	53.28±32.97^*
SIRS group (n=32)	152.61±69.23^*	13.14±1.93^*	37.87±12.31^*	866.00 (143-1 894)^*	51.78±31.57^*
Control group (n=20)	230.60±20.00	10.66±0.66	21.22±2.51	193.50 (56-350)	104.52±15.05
F value	4.010	8.172	10.442	12.089	12.103
P value	0.011	0.001	0.000	0.002	0.000

Variables	Platelet count	PT	APTT	D-dimer	AT-III
CRP (rvalue)	-0.417	0.562	0.558	0.585	-0.315
P value	0.000	0.000	0.000	0.000	0.010
TNF-α (rvalue)	-0.444	0.510	0.409	0.502	-0.277
P value	0.000	0.000	0.000	0.000	0.024

s-CD62P	Inflammatory factors		Coagulation indexes
s-CD62P	CRP	TNF-α	Platelet count	PT	APTT	D-dimer	AT-III
r value	0.818	0.694	-0.347	0.451	0.377	0.423	-0.239
P value	0.000	0.000	0.003	0.000	0.001	0.000	0.050