Delving into the Latest Updates on DW-1029M with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

DW 1029M

Target

Advanced glycation end product x TGF-β1

Action

inhibitors

Mechanism

Advanced glycation end product inhibitors, TGF-β1 inhibitors(Transforming growth factor beta 1 inhibitors)

Therapeutic Areas

Endocrinology and Metabolic DiseaseUrogenital Diseases

Active Indication-

Inactive Indication

Diabetic Nephropathies

Originator Organization

DONG WHA PHARM Co., Ltd.

Active Organization-

Inactive Organization

DONG WHA PHARM Co., Ltd.

License Organization-

Drug Highest PhasePendingPhase 2

First Approval Date-

Regulation-

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DW1029M is a botanical extract of Morus albalinne root bark and Puerariae radix that is used for the treatment of diabetic nephropathy. This study evaluated the safety and pharmacokinetics of DW1029M following its administration in healthy Korean subjects. We conducted a randomized, open‐label, single‐dose, crossover phase 1 clinical study. During each period, subjects received 300, 600, or 1200 mg oral doses of DW1029M. Plasma concentrations of puerarin, daidzin, and daidzein were analyzed using a liquid chromatography–tandem mass spectrometry. Six healthy male subjects completed the study. The maximum concentration of the drug in the plasma (Cmax) and area under the plasma drug concentration–time curve to the last measurable concentration (AUClast) for puerarin, daidzin, and daidzein were assessed after oral administration of DW1029M. No serious adverse events or clinically or statistically significant adverse events associated with any of the drug levels were observed. The results of the measurement of vital signs, electrocardiogram, laboratory tests, and physical examinations indicated that no clinically significant changes occurred during this study. The DW1029M tablet was safe and well tolerated over a single dose range of 300–1200 mg. This pharmacokinetic study of a botanical drug may aid in the development of DW1029M.

01 Jul 2017·Clinical pharmacology in drug development

Phase 1 and Pharmacokinetic Drug–Drug Interaction Study of Metformin, Losartan, and Linagliptin Coadministered With DW1029M in Healthy Volunteers

Article

Author: Jeon, Ji‐Young ; Lim, Cheol‐Hee ; Kim, Min‐Gul ; Jang, Hwan Bong ; Moon, Seol Ju ; Kim, Sun‐Young

Abstract:

We investigated botanical drug–pharmaceutical drug interactions between DW1029M (a botanical extract ofMorus alba linneroot bark andPuerariae radix) and metformin, losartan, and linagliptin in the steady state. Three studies were conducted as randomized, open‐label, 2‐period, 2‐treatment, multiple‐dose, 2‐way crossover designs. Eligible subjects received metformin (500 mg twice daily), losartan (50 mg once daily), or linagliptin (5 mg once daily) with DW1029M (300 mg × 2T twice daily) every 12 hours on days 1 through 6 and a single dose on the morning of day 7. Coadministration of DW1029M with metformin, losartan, or linagliptin had no clinically relevant effects based on the area under the plasma concentration–time curve (AUCτ) geometric least‐squares mean ratio (GMR) — AUCτGMR, 89.7; 90% confidence interval (CI), 81.0–99.4 for metformin; AUCτGMR, 96.2; 90%CI, 86.3–107.1 for losartan; and AUCτGMR, 89.7; 90%CI, 83.2–96.6 for linagliptin. In addition, coadministration of DW1029M did not have any clinically meaningful effect on the maximum plasma concentration (Cmax,ss) — Cmax,ssGMR, 87.3; 90%CI, 76.2–100.0 for metformin; Cmax,ssGMR, 90.5; 90%CI, 78.3–104.6 for losartan; and Cmax,ssGMR, 81.4; 90%CI, 69.5–95.3 for linagliptin. Coadministration of DW1029M with metformin, losartan, or linagliptin was well tolerated.

15 May 2014·American journal of physiology. Renal physiologyQ3 · MEDICINE

DW1029M, a novel botanical drug candidate, inhibits advanced glycation end-product formation, rat lens aldose reductase activity, and TGF-β₁signaling

Q3 · MEDICINE

Article

Author: Yoon, Joobyoung ; Choi, Hyunsik ; Chang, Hwan Bong ; Choi, Dong Hwa ; Ku, Bonchul ; Park, Dongeun ; Lee, Hyunyong ; Seong, Seungkyoo ; Rho, Yang Kook ; Kim, Yong Sung

DW1029M is a botanical extract consisting of Morus bark and Puerariae radix, produced by Dong-Wha Pharmaceutical, for nephroprotective drug development; it has been in phase II clinical trials in Korea. In our mechanistic investigations, we found that DW1029M inhibits advanced glycation end products (AGEs), rat lens aldose reductase (RLAR), and transforming growth factor (TGF)-β1signaling, all of which are implicated in diabetic complications such as diabetic nephropathy and diabetic retinopathy. DW1029M inhibits AGE formation via Fe2+chelation. The extract contains 13 active constituents that inhibit AGE formation, 8 active constituents that inhibit RLAR activity, and 1 inhibitor of TGF-β1signaling. Our results suggest DW1029M protects against diabetic nephropathy via blockade of AGE formation, RLAR activity, and TGF-β1signaling.

100 Deals associated with DW-1029M

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