Research progress on clinical application of anti-tissue factor pathway inhibitor in hemophilia

doi:10.16150/j.1671-2870.2025.02.015

Abstract

Abstract:

In recent years， to address the unmet needs in hemophilia treatment， significant research has led to unprecedented advances in pharmacotherapy， including the development of several innovative mechanism-based therapies that restore hemostatic balance by modulating thrombin generation in hemophilia patients with or without inhibitors. Among them， non-factor therapies involving hemostatic rebalancing mechanisms have achieved remarkable progress， with one of the key focuses in clinical development being anti-tissue factor pathway inhibitor （TFPI） therapy. TFPI is a key anticoagulant protein in the coagulation pathway that inhibits tissue factor （TF）-mediated initiation of coagulation. Blocking TFPI activity can enhance thrombin generation， providing a novel approach for hemophilia treatment. Notably， this mechanism applies to patients with hemophilia A or B and is theoretically effective for patients with or without inhibitors. As of June 2025， anti-TFPI agents that have entered clinical development or been approved for marketing internationally include concizumab， marstacimab， befovacimab， KN057， and MG1113. These agents inhibit TFPI activity through different antibody types， employing varying binding affinities or targeting distinct domains of TFPI. Studies on clinical trials across various phases have demonstrated that these drugs have good efficacy in reducing annual bleeding rates and improving patient prognosis. In addition， anti-TFPI drugs are administered subcutaneously， with dosing intervals up to one week， providing convenience for patients. Anti-TFPI therapy represents an important shift in the field of hemophilia management. However， it faces some challenges， including potential thrombotic risks and the current absence of suitable laboratory assays to monitor treatment efficacy.

Key words: Hemophilia, Anti-tissue factor pathway inhibitor, Thrombosis

CLC Number:

R554⁺.1

XIAO Jianwen, YI Weijia. Research progress on clinical application of anti-tissue factor pathway inhibitor in hemophilia[J]. Journal of Diagnostics Concepts & Practice, 2025, 24(02): 226-232.

Figures/Tables 2

Figure 1

Table 1

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抗TFPI单克隆抗体	单克隆抗体特性	TFPI结合位点	最新临床开发阶段		全球上市情况
抗TFPI单克隆抗体	单克隆抗体特性	TFPI结合位点	NCT编号	受试者形态	全球上市情况
concizumab	人源化IgG 4	K2结构域	NCT04083781 (explorer 7)	12岁及以上患有血友病A或血友病B并伴有抑制物的患者（任何严重程度）	加拿大 (2023)^* 瑞士 (2023)^* 澳洲 (2023)^* 日本 (2023)^† 美国 (2024)^¶
			NCT04082429 (explorer8)	12岁及以上患有血友病A或血友病B未伴有抑制物的患者
			NCT05135559 进行中 (explorer10)	12岁以下A型或B型血友病患者，伴有或不伴有抑制物
marstacimab	全人源IgG1	K2结构域	NCT03938792 (BASIS)	12岁及以上A型（重型）或B型（中重型至重型）血友病患者，伴有或不伴有抑制物	美国 (2024)^‡ 欧盟 (2024)^§ 2024年8月13日在中国申报上市并获得受理。
marstacimab	全人源IgG1	K2结构域	NCT05611801 (BASIS KIDS)	12岁以下A型（重型）或B型（中重型至重型）血友病患者，伴有或不伴有抑制物	美国 (2024)^‡ 欧盟 (2024)^§ 2024年8月13日在中国申报上市并获得受理。
befovacimab	人源化IgG2	K1和K2结构域	Ⅱ期 NCT03597022 终止	18岁及以上A型或B型血友病患者，伴有或不伴有抑制物
KN057	人源化		Ⅲ期 NCT06312475进行中	12岁及以上患有血友病A或血友病B并伴有抑制物的患者
MG1113	人源化IgG4	K2结构域	Ⅰb期 NCT05493631进行中	19岁及以上重型血友病A或血友病B患者，伴有或不伴有抑制物