皮下或静脉注射治疗剂量的普通肝素（200 U/kg）给健康犬后的药代动力学和药效学。

Pharmacokinetics and pharmacodynamics of a therapeutic dose of unfractionated heparin (200 U/kg) administered subcutaneously or intravenously to healthy dogs.

作者信息

Diquélou A, Barbaste C, Gabaig A M, Trumel C, Abella-Bourges N, Guelfi J-F, Bousquet Mélou A

机构信息

Ecole Nationale Vétérinaire de Toulouse, Toulouse, France.

出版信息

Vet Clin Pathol. 2005 Sep;34(3):237-42. doi: 10.1111/j.1939-165x.2005.tb00047.x.

DOI:10.1111/j.1939-165x.2005.tb00047.x

PMID:16134071

Abstract

BACKGROUND

Heparin treatment has been recommended for dogs in hypercoagulable states such as disseminated intravascular coagulation, however, potential benefits have to be balanced against the bleeding risk if overdosage occurs. A better understanding of the pharmacology of heparin and tests to monitor heparin therapy in dogs may help prevent therapeutic hazards.

OBJECTIVES

The purpose of this study was to evaluate the effects of 200 U/kg of sodium unfractionated heparin (UFH) on coagulation times in dogs after intravenous (IV) and subcutaneous (SC) administration and to compare these effects with plasma heparin concentrations assessed by its antifactor Xa (aXa) activity.

METHODS

200 U/kg of UFH were administered IV and SC to 5 healthy adult Beagle dogs with a washout period of at least 3 days. Activated partial thromboplastin time (APTT), prothrombin time (PT), and plasma aXa activity were determined in serial blood samples.

RESULTS

After IV injection, PT remained unchanged except for a slight increase in 1 dog; APTT was not measurable (>60 seconds) for 45-90 minutes, and then decreased gradually to baseline values between 150 and 240 minutes. High plasma heparin concentrations were observed (maximal concentration = 4.64 +/-1.4 aXa U/mL) and decreased according to a slightly concave-convex pattern on a semilogarithmic curve, but returned to baseline slightly more slowly (t240-t300 minutes) than did APTT. After SC administration, APTT was moderately prolonged (by a ratio of 1.55 +/-0.28 APTT t0, range 1.35-2.01) between 1 and 4 hours after administration. Plasma aXa activity reached a maximum of 0.56 +/-0.20 aXa U/mL (range 0.42-0.9 U/mL) after 132 +/-26.8 minutes; this lasted for 102 +/-26.8 minutes. Prolongation of APTTs of 120-160% corresponded to plasma heparin concentrations of 0.3-0.7 aXa U/mL.

CONCLUSIONS

As in humans, the pharmacokinetics of UFH in dogs was nonlinear. Administration of 200 U/kg of UFH SC in healthy dogs resulted in sustained plasma heparin concentrations in accordance with human recommendations for thrombosis treatment or prevention, without excessively increased bleeding risks. In these conditions, APTT can be used as a surrogate to assess plasma heparin concentrations. These findings need to be confirmed in diseased animals.

摘要

背景

对于处于高凝状态（如弥散性血管内凝血）的犬类，已推荐使用肝素治疗，然而，如果用药过量，必须在潜在益处与出血风险之间进行权衡。更好地了解肝素的药理学以及监测犬类肝素治疗的检测方法可能有助于预防治疗风险。

目的

本研究的目的是评估200 U/kg普通肝素钠（UFH）静脉注射（IV）和皮下注射（SC）后对犬类凝血时间的影响，并将这些影响与通过抗Xa因子（aXa）活性评估的血浆肝素浓度进行比较。

方法

将200 U/kg的UFH静脉注射和皮下注射给5只健康成年比格犬，洗脱期至少为3天。在系列血样中测定活化部分凝血活酶时间（APTT）、凝血酶原时间（PT）和血浆aXa活性。

结果

静脉注射后，除1只犬略有增加外，PT保持不变；APTT在45 - 90分钟内无法测量（>60秒），然后在150至240分钟之间逐渐降至基线值。观察到血浆肝素浓度较高（最大浓度 = 4.64 +/-1.4 aXa U/mL），并在半对数曲线上呈略凹凸的模式下降，但恢复到基线的速度比APTT略慢（t240 - t300分钟）。皮下注射后，给药后1至4小时内APTT中度延长（APTT t0的比值为1.55 +/-0.28，范围为1.35 - 2.01）。血浆aXa活性在132 +/-26.8分钟后达到最大值0.56 +/-0.20 aXa U/mL（范围为0.42 - 0.9 U/mL）；持续102 +/-26.8分钟。APTT延长120 - 160%对应血浆肝素浓度为0.3 - 0.7 aXa U/mL。