Moroctocog alfa

DB13999

biotech approved

Deskripsi

Moroctocog alfa, also known as BDDrFVIII (B domain deleted recombinant factor VIII), is a recombinant DNA-based drug with functional characteristics comparable to those of endogenous coagulation Factor VIII, the essential human blood clotting protein that is impaired in Hemophilia A. Moroctocog alfa is identical in sequence to endogenously produced Factor VIII, but does not contain the B-domain, which has no known biological function. Moroctocog alfa is produced through recombinant DNA technology and purification, resulting in a 1438 amino acid, 170 kDa protein FDA Label. Clinical evaluation has shown that BDDrFVIII is pharmacokinetically equivalent to full-length recombinant FVIII A32468, FDA Label.

Also known as Anti-Hemophilic Factor (AHF), endogenous Factor VIII is essential to the clotting process in the body due to its involvement in the clotting cascade where it is responsible for acting as a co-factor to Factor IX. Activation of Factor IX leads to a cascade of signals that results in activation of Factor X, which then results in the conversion of prothrombin to thrombin, and as a result, leads to the conversion of fibrinogen to fibrin, the fibrous protein that creates the scaffold of the clot. Replacement of Factor VIII is essential for the treatment of Hemophilia A, which is caused by mutations in the Factor VIII gene, leading to a functional deficiency or complete loss of protein. Congenital loss or deficiency of Factor VIII results in the physiologic impairment of the coagulation clotting cascade, and as a result, leads to easy bruising and bleeding. Bleeding can range in severity from minor concerns, such as nosebleeds, to more serious events such as hemorrhaging in the joints, brain, or digestive tract ^A32280.

Exogenous replacement of Factor VIII is currently the cornerstone of Hemophilia treatment and is used for the prophylaxis and control of bleeding episodes. Treatment has drastically improved since the 1960s when Factor VIII protein was primarily purified from human plasma, rather than being produced through recombinant DNA technology. Unfortunately, purification of protein from human plasma carries an increased risk of transmission of blood-borne diseases such as HIV and Hepatitis, which in part contributed to the Tainted Blood Scandal in the 1980s A31551, A32272, L2177. Use of recombinant DNA-derived clotting factor treatments, such as Moroctocog alfa, has reduced this risk.

Other drug products with similar structure and function to Moroctocog alfa include DB13192, which is purified Factor VIII from human pooled blood and contains both A- and B-subunits, and DB11607, which is a fully recombinant factor VIII-Fc fusion protein which has an extended half-life compared with conventional factor VIII due to conjugation to the dimeric Fc domain of human immunoglobulin G1, a long-lived plasma protein ^A31551.

Moroctocog alfa is approved by Health Canada and by the European Medicines Agency for the control and prevention of hemorrhagic episodes and for routine and surgical prophylaxis in patients with hemophilia A (congenital factor VIII deficiency or classic hemophilia). As it does not contain von Willebrand factor it is not indicated in von Willebrand’s disease FDA Label.

Struktur Molekul 2D

Struktur tidak tersedia

Peta Jejaring Molekuler

Obat Target Gen Interaksi Enzim Transporter Carrier

Legenda: Obat • Target • Gen • Enzim • (Panah → menunjukkan arah efek / relasi) • Transporter • Carrier

1. Pendahuluan & Konsep

Fitur visualisasi ini dikembangkan menggunakan pendekatan Graph Theory untuk memetakan hubungan polifarmasi dan molekuler. Entitas (Obat, Target, Gen) direpresentasikan sebagai Simpul (Nodes), sedangkan hubungan biologisnya sebagai Sisi (Edges).

2. Sumber Data (Validasi)

Data Obat: Diekstraksi dari elemen drugbank-id dan name pada skema XML DrugBank.
Target Protein: Diambil dari elemen targets/target yang memuat polipeptida sasaran.
Genetik: Disinkronisasi dari sub-elemen gene-name dan varian snp-effects.
Genetik: Jumlah titik node dibatasi pada maksimal 10 (Slice=10) interaksi untuk menghindari tumpukan data.

3. Algoritma Visualisasi

Tata letak grafik menggunakan algoritma Force-Directed Graph (Barnes-Hut). Model fisika ini menerapkan gaya tolak-menolak antar simpul (Gravitasi: -3000) agar tidak tumpang tindih, serta gaya pegas (Spring: 0.04) pada garis penghubung untuk fleksibilitas interaksi.

4. Legenda Visual

Obat Utama (Pusat Analisis)

Target Protein (Mekanisme)

Gen (Faktor Genetik)

Metode ini mendukung analisis Precision Medicine dan evaluasi risiko Drug-Drug Interaction (DDI).

Profil Farmakokinetik

Waktu Paruh (Half-Life) Mean terminal elimination half-life = 11.8 (± 5.1) hours [FDA Label] Half-life = 11.2 ± 5.0 hours [A32468]

Volume Distribusi Mean steady-state volume of distribution = 65.1 (± 35.1) mL/kg [FDA Label]

Klirens (Clearance) Mean clearance = 4.21 (± 2.08) mL/h•kg [FDA Label] Clearance = 4.51 ± 2.23 mL/h•kg [A32468]

Absorpsi

Cmax = 1.08±0.22 IU?hr/mL ^A32468 Cmax = 1.12 (±0.19) IU/mL FDA Label

Metabolisme

Data metabolisme tidak tersedia.

Rute Eliminasi

Data eliminasi belum tersedia.

Interaksi Obat

92 Data

Aminocaproic acid	The risk or severity of adverse effects can be increased when Aminocaproic acid is combined with Moroctocog alfa.
Alpha-1-proteinase inhibitor	Alpha-1-proteinase inhibitor may increase the thrombogenic activities of Moroctocog alfa.
Menadione	Menadione may increase the thrombogenic activities of Moroctocog alfa.
Tranexamic acid	Tranexamic acid may increase the thrombogenic activities of Moroctocog alfa.
Aprotinin	Aprotinin may increase the thrombogenic activities of Moroctocog alfa.
Hydrogen peroxide	Hydrogen peroxide may increase the thrombogenic activities of Moroctocog alfa.
Aminomethylbenzoic acid	Aminomethylbenzoic acid may increase the thrombogenic activities of Moroctocog alfa.
Camostat	Camostat may increase the thrombogenic activities of Moroctocog alfa.
Menadione bisulfite	Menadione bisulfite may increase the thrombogenic activities of Moroctocog alfa.
Monteplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Monteplase.
Lepirudin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Lepirudin.
Bivalirudin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Bivalirudin.
Alteplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Alteplase.
Urokinase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Urokinase.
Reteplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Reteplase.
Anistreplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Anistreplase.
Tenecteplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Tenecteplase.
Abciximab	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Abciximab.
Drotrecogin alfa	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Drotrecogin alfa.
Streptokinase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Streptokinase.
Dicoumarol	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dicoumarol.
Argatroban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Argatroban.
Ardeparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Ardeparin.
Phenindione	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Phenindione.
Fondaparinux	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Fondaparinux.
Warfarin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Warfarin.
Pentosan polysulfate	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Pentosan polysulfate.
Phenprocoumon	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Phenprocoumon.
Dipyridamole	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dipyridamole.
Heparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Heparin.
Enoxaparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Enoxaparin.
Epoprostenol	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Epoprostenol.
Acenocoumarol	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Acenocoumarol.
4-hydroxycoumarin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with 4-hydroxycoumarin.
Coumarin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Coumarin.
Ximelagatran	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Ximelagatran.
Desmoteplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Desmoteplase.
Defibrotide	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Defibrotide.
Ancrod	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Ancrod.
Beraprost	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Beraprost.
Prasugrel	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Prasugrel.
Rivaroxaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Rivaroxaban.
Sulodexide	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Sulodexide.
Idraparinux	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Idraparinux.
Cangrelor	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Cangrelor.
Astaxanthin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Astaxanthin.
Apixaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Apixaban.
Otamixaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Otamixaban.
Amediplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Amediplase.
Dabigatran etexilate	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dabigatran etexilate.
Danaparoid	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Danaparoid.
Dalteparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dalteparin.
Tinzaparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Tinzaparin.
(R)-warfarin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with (R)-warfarin.
Ethyl biscoumacetate	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Ethyl biscoumacetate.
Nadroparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Nadroparin.
Triflusal	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Triflusal.
Ticagrelor	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Ticagrelor.
Ditazole	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Ditazole.
Vorapaxar	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Vorapaxar.
Edoxaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Edoxaban.
Sodium citrate	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Sodium citrate.
Dextran	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dextran.
Bemiparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Bemiparin.
Parnaparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Parnaparin.
Desirudin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Desirudin.
Antithrombin Alfa	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Antithrombin Alfa.
Protein C	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Protein C.
Antithrombin III human	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Antithrombin III human.
Letaxaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Letaxaban.
Darexaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Darexaban.
Betrixaban	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Betrixaban.
Nafamostat	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Nafamostat.
Gabexate	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Gabexate.
Fluindione	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Fluindione.
Protein S human	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Protein S human.
Brinase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Brinase.
Clorindione	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Clorindione.
Diphenadione	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Diphenadione.
Tioclomarol	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Tioclomarol.
Melagatran	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Melagatran.
Saruplase	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Saruplase.
(S)-Warfarin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with (S)-Warfarin.
Tocopherylquinone	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Tocopherylquinone.
Dabigatran	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dabigatran.
Semuloparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Semuloparin.
Troxerutin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Troxerutin.
Edetic acid	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Edetic acid.
Reviparin	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Reviparin.
Dermatan sulfate	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Dermatan sulfate.
SR-123781A	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with SR-123781A.
Limaprost	The therapeutic efficacy of Moroctocog alfa can be decreased when used in combination with Limaprost.

Target Protein

Coagulation factor X F10

Coagulation factor IX F9

von Willebrand factor VWF

Phytanoyl-CoA dioxygenase, peroxisomal PHYH

Asialoglycoprotein receptor 2 ASGR2

Endoplasmic reticulum chaperone BiP HSPA5

Calreticulin CALR

Calnexin CANX

Protein ERGIC-53 LMAN1

Prolow-density lipoprotein receptor-related protein 1 LRP1

Multiple coagulation factor deficiency protein 2 MCFD2

Referensi & Sumber

Artikel (PubMed)

PMID: 2157
Titheradge MA, Coore HG: Initial rates of pyruvate transport in mitochondria determined by an "inhibitor-stop" technique. Biochem J. 1975 Sep;150(3):553-6.
PMID: 25548513
Santagostino E: A new recombinant factor VIII: from genetics to clinical use. Drug Des Devel Ther. 2014 Dec 12;8:2507-15. doi: 10.2147/DDDT.S73241. eCollection 2014.
PMID: 27487799
Frampton JE: Efmoroctocog Alfa: A Review in Haemophilia A. Drugs. 2016 Sep;76(13):1281-1291. doi: 10.1007/s40265-016-0622-z.
PMID: 23815950
Franchini M, Mannucci PM: Hemophilia A in the third millennium. Blood Rev. 2013 Jul;27(4):179-84. doi: 10.1016/j.blre.2013.06.002. Epub 2013 Jun 28.
PMID: 19473411
Recht M, Nemes L, Matysiak M, Manco-Johnson M, Lusher J, Smith M, Mannucci P, Hay C, Abshire T, O'Brien A, Hayward B, Udata C, Roth DA, Arkin S: Clinical evaluation of moroctocog alfa (AF-CC), a new generation of B-domain deleted recombinant factor VIII (BDDrFVIII) for treatment of haemophilia A: demonstration of safety, efficacy, and pharmacokinetic equivalence to full-length recombinant factor VIII. Haemophilia. 2009 Jul;15(4):869-80. doi: 10.1111/j.1365-2516.2009.02027.x. Epub 2009 Apr 9.

Link

Contoh Produk & Brand

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Sekuens Gen/Protein (FASTA)

Sekuens dimuat saat dibutuhkan agar halaman tetap ringan.