Central Venous Catheter Thrombosis Clinical Trial
Official title:
The Relationship Between the Lack of Plasma Antithrombin Ⅲ, Protein C, Protein S Activity and Peripherally Inserted Central Catheter Related Thrombosis
PICC related venous thrombosis (PICC-RVT) is one of the common complications of PICC and the main cause of unplanned extubation. Effectively identifying the risk of PICC-RVT in patients and preventing PICC-RVT are of great clinical significance. There are many studies on the risk factors of VTE at home and abroad, and there are also many studies on the risk assessment of PICC catheter-related thrombosis, mostly focusing on sociodemographic data, comorbidities, and intubation related factors, while the research on laboratory related indicators is limited It involves D-dimer, white blood cell count (WBC), platelet count (PLT), etc., but its specificity or positive predictive value is not high, and there is no reliable biomarker report. Studies have shown that the decrease or lack of AT-Ⅲ, PC, PS activity is one of the mechanisms of hypercoagulable state in patients with cancer, and may be a biomarker of thrombosis. Many retrospective studies have also shown that the activities of AT-Ⅲ, PC, and PS are related to the occurrence and recurrence of VTE and DVT. The pathogenesis is mainly anticoagulant protein defect or decreased expression. However, when PICC is implanted in patients with AT-Ⅲ, PC and PS activity defects, whether PICC indwelling will become a predisposing factor of thrombosis is not yet known. Therefore, the purpose of this study is to understand the rate of anticoagulant protein deficiency in patients with tumor PICC-RVT, and to prospectively explore the correlation between the lack of AT-Ⅲ, PC, and PS activities and PICC-RVT, and to provide targeted preventive interventions for PICC-RVT patients Scientific basis.
A prospective study showed that a mild reduction in AT levels (70%-80%) was associated with
the recurrence of no incentive VTE. Subsequent studies defined mild AT deficiency as less
than the 5th percentile of the normal range to further verify that mild AT deficiency is a
risk factor for VTE recurrence. Many retrospective studies have also shown that the
activities of AT-Ⅲ, PC and PS are related to the occurrence and recurrence of VTE and DVT.
Taking the lower limit of the normal reference value as the criterion for judging the lack of
anticoagulant protein activity, Zhu Tienan et al. found that the lack of activity of AT, PC,
and PS in normal people were 1.15%, 1.49%, and 2.29%, respectively. Fang Biqian et al. found
277 cases of VTE. Among the cases found that the lack of activity of AT, PC, and PS were
16.00%, 17.45%, and 17.09%, respectively. That is, the lack of activity of the three
anticoagulant proteins in VTE patients was about 10 times higher than that of normal people.
Chinese scholars from Taiwan, Hong Kong and Shanghai also found that the total lack of three
anticoagulant proteins of AT-Ⅲ, PC and PS exceeds 15% in Western countries, suggesting that
the etiological composition of venous thromboembolism in the Chinese population may be
similar to that of Western countries. Different, reflecting that anticoagulant protein
deficiency plays an important role in the pathogenesis of VTE patients in China. Compared
with factor V Leiden mutation and prothrombin 20210A mutation, the most common thrombosis in
Asian population is antithrombin Ⅲ (AT-Ⅲ), protein C (protein C, PC) and protein S (protein
S, PS), etc. Defects of anticoagulant protein. When the hypercoagulable state caused by
anticoagulant protein deficiency is induced by certain risk factors for thrombosis, such as
pregnancy, oral contraceptives, fractures, long-term immobilization, etc., it can lead to the
occurrence of VTE. When PICC is implanted in patients with AT-Ⅲ, PC and PS activity defects,
whether PICC indwelling will become a predisposing factor of thrombosis is not yet known.
It has been reported that the severity of CVC-related thrombosis in patients with AT-Ⅲ
deficiency after CVC catheterization is higher than that of the normal group. Nowak-Göttl et
al. showed that PC and PS genetic defects are related to catheterization in children
Thrombosis plays an important role. In 2016, a systematic review showed that the risk of DVT
related to more than one anticoagulant defect increased by 3.20 times. PC defects can
increase the incidence of CVC-related DVT in children. Our preliminary study of this subject
found that the lack of anticoagulant protein in PICC-RVT patients was higher than that in
non-PICC-RVT patients.
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