Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies

Rupert Bauersachs; Florian Langer; Christoph Kalka; Stavros Konstantinides; Robert Klamroth; Johannes Oldenburg; Sebastian Schellong; Ute Scholz; Markus Stücker; Edelgard Lindhoff-Last

doi:10.1024/0301-1526/a000815

Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies

Standard

Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies. / Bauersachs, Rupert; Langer, Florian; Kalka, Christoph; Konstantinides, Stavros; Klamroth, Robert; Oldenburg, Johannes; Schellong, Sebastian; Scholz, Ute; Stücker, Markus; Lindhoff-Last, Edelgard.

in: VASA, Jahrgang 48, Nr. 6, 11.2019, S. 483-486.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Bauersachs, R, Langer, F, Kalka, C, Konstantinides, S, Klamroth, R, Oldenburg, J, Schellong, S, Scholz, U, Stücker, M & Lindhoff-Last, E 2019, 'Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies', VASA, Jg. 48, Nr. 6, S. 483-486. https://doi.org/10.1024/0301-1526/a000815

APA

Bauersachs, R., Langer, F., Kalka, C., Konstantinides, S., Klamroth, R., Oldenburg, J., Schellong, S., Scholz, U., Stücker, M., & Lindhoff-Last, E. (2019). Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies. VASA, 48(6), 483-486. https://doi.org/10.1024/0301-1526/a000815

Vancouver

Bauersachs R, Langer F, Kalka C, Konstantinides S, Klamroth R, Oldenburg J et al. Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies. VASA. 2019 Nov;48(6):483-486. https://doi.org/10.1024/0301-1526/a000815

Bibtex

@article{5c1024359c0e44af949f48e2434ab1bf,

title = "Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies",

abstract = " The antiphospholipid-syndrome (APS) is one of the most severe forms of thrombophilia, which may not only lead to recurrent venous but also to arterial thromboembolic events (TE), and to severe pregnancy complications, respectively. APS is defined by clinical symptoms and specific laboratory findings: 1. Lupus anticoagulant (LA), 2. anticardiolipin-antibodies (ACA), and 3. β2-Glycoprotein I-antibodies (β2GPI-Ab). All test results have to be confirmed after at least 12 weeks. The thrombotic risk is highest, if all 3 test groups are positive. It must be pointed out that the presence of UFH, VKA or DOACs may lead to false positive LA-test results; the addition of a specific absorber after blood sampling may provide reliable results in the presence of DOACs. A prospective randomized controlled trial comparing warfarin and rivaroxaban (TRAPS-trial) including only high-risk patients with triple positive APS was terminated early because of an increased rate of TE in patients treated with rivaroxaban [19 %, mostly arterial, compared to 3 % with warfarin (HR 7.4;1.7-32.9)]. Subsequently, a warning letter was issued by the pharmaceutical manufacturers of DOACs, including a warning of DOAC use in APS-patients, particularly in triple-positive high-risk patients. Conclusions: 1. Clinical suspicion of APS requires careful diagnostic testing. Because of inadequate diagnostic workup, many patients may not even have an APS, and these patients could be adequately treated with a DOAC. 2. Patients with single or double positive antiphospholipid antibodies but without positive LA may have a comparably low thrombotic risk and may also be treated with a DOAC in venous TE - sufficient evidence for that conclusion is not yet available but is suggested by the results of meta-analyses. 3. Triple positive patients or those with APS who suffered from arterial thromboembolism have a very high recurrence risk of thrombosis; the TRAPS-Study shows that these patients should be treated with VKA instead of a DOAC.",

keywords = "Anticoagulants/therapeutic use, Antiphospholipid Syndrome/drug therapy, Humans, Prospective Studies, Rivaroxaban/therapeutic use, Warfarin/therapeutic use",

author = "Rupert Bauersachs and Florian Langer and Christoph Kalka and Stavros Konstantinides and Robert Klamroth and Johannes Oldenburg and Sebastian Schellong and Ute Scholz and Markus St{\"u}cker and Edelgard Lindhoff-Last",

year = "2019",

month = nov,

doi = "10.1024/0301-1526/a000815",

language = "English",

volume = "48",

pages = "483--486",

journal = "VASA",

issn = "0301-1526",

publisher = "Hans Huber",

number = "6",

}

RIS

TY - JOUR

T1 - Treatment of the antiphospholipid syndrome with direct oral anticoagulants Position statement of German societies

AU - Bauersachs, Rupert

AU - Langer, Florian

AU - Kalka, Christoph

AU - Konstantinides, Stavros

AU - Klamroth, Robert

AU - Oldenburg, Johannes

AU - Schellong, Sebastian

AU - Scholz, Ute

AU - Stücker, Markus

AU - Lindhoff-Last, Edelgard

PY - 2019/11

Y1 - 2019/11

N2 - The antiphospholipid-syndrome (APS) is one of the most severe forms of thrombophilia, which may not only lead to recurrent venous but also to arterial thromboembolic events (TE), and to severe pregnancy complications, respectively. APS is defined by clinical symptoms and specific laboratory findings: 1. Lupus anticoagulant (LA), 2. anticardiolipin-antibodies (ACA), and 3. β2-Glycoprotein I-antibodies (β2GPI-Ab). All test results have to be confirmed after at least 12 weeks. The thrombotic risk is highest, if all 3 test groups are positive. It must be pointed out that the presence of UFH, VKA or DOACs may lead to false positive LA-test results; the addition of a specific absorber after blood sampling may provide reliable results in the presence of DOACs. A prospective randomized controlled trial comparing warfarin and rivaroxaban (TRAPS-trial) including only high-risk patients with triple positive APS was terminated early because of an increased rate of TE in patients treated with rivaroxaban [19 %, mostly arterial, compared to 3 % with warfarin (HR 7.4;1.7-32.9)]. Subsequently, a warning letter was issued by the pharmaceutical manufacturers of DOACs, including a warning of DOAC use in APS-patients, particularly in triple-positive high-risk patients. Conclusions: 1. Clinical suspicion of APS requires careful diagnostic testing. Because of inadequate diagnostic workup, many patients may not even have an APS, and these patients could be adequately treated with a DOAC. 2. Patients with single or double positive antiphospholipid antibodies but without positive LA may have a comparably low thrombotic risk and may also be treated with a DOAC in venous TE - sufficient evidence for that conclusion is not yet available but is suggested by the results of meta-analyses. 3. Triple positive patients or those with APS who suffered from arterial thromboembolism have a very high recurrence risk of thrombosis; the TRAPS-Study shows that these patients should be treated with VKA instead of a DOAC.

AB - The antiphospholipid-syndrome (APS) is one of the most severe forms of thrombophilia, which may not only lead to recurrent venous but also to arterial thromboembolic events (TE), and to severe pregnancy complications, respectively. APS is defined by clinical symptoms and specific laboratory findings: 1. Lupus anticoagulant (LA), 2. anticardiolipin-antibodies (ACA), and 3. β2-Glycoprotein I-antibodies (β2GPI-Ab). All test results have to be confirmed after at least 12 weeks. The thrombotic risk is highest, if all 3 test groups are positive. It must be pointed out that the presence of UFH, VKA or DOACs may lead to false positive LA-test results; the addition of a specific absorber after blood sampling may provide reliable results in the presence of DOACs. A prospective randomized controlled trial comparing warfarin and rivaroxaban (TRAPS-trial) including only high-risk patients with triple positive APS was terminated early because of an increased rate of TE in patients treated with rivaroxaban [19 %, mostly arterial, compared to 3 % with warfarin (HR 7.4;1.7-32.9)]. Subsequently, a warning letter was issued by the pharmaceutical manufacturers of DOACs, including a warning of DOAC use in APS-patients, particularly in triple-positive high-risk patients. Conclusions: 1. Clinical suspicion of APS requires careful diagnostic testing. Because of inadequate diagnostic workup, many patients may not even have an APS, and these patients could be adequately treated with a DOAC. 2. Patients with single or double positive antiphospholipid antibodies but without positive LA may have a comparably low thrombotic risk and may also be treated with a DOAC in venous TE - sufficient evidence for that conclusion is not yet available but is suggested by the results of meta-analyses. 3. Triple positive patients or those with APS who suffered from arterial thromboembolism have a very high recurrence risk of thrombosis; the TRAPS-Study shows that these patients should be treated with VKA instead of a DOAC.

KW - Anticoagulants/therapeutic use

KW - Antiphospholipid Syndrome/drug therapy

KW - Humans

KW - Prospective Studies

KW - Rivaroxaban/therapeutic use

KW - Warfarin/therapeutic use

U2 - 10.1024/0301-1526/a000815

DO - 10.1024/0301-1526/a000815

M3 - SCORING: Journal article

C2 - 31621546

VL - 48

SP - 483

EP - 486

JO - VASA

JF - VASA

SN - 0301-1526

IS - 6

ER -