A total of 65 patients completed the study, in which DUR-928 was orally administered daily for 4 weeks at 50 mg (n=23), 150 mg (n=21), or 600 mg (300 mg BID (n=21)). Both the 50 mg and 600 mg dose groups showed a statistically significant median reduction at day 28 from baseline of serum alanine aminotransferase (ALT) levels at -16% and -17%, respectively. The 600 mg dose group also showed statistically significant median reductions at day 28 from baseline of serum aspartate aminotransferase (AST) (-18%) and gamma-glutamyl transferase (GGT) (-8%), and the 50 mg dose group had a statistically significant reduction at day 28 from baseline in liver stiffness as measured by Fibroscan (-10%).
Patients in the 50 mg or 150 mg dose groups also had statistically significant median reduction at day 28 from baseline of serum triglycerides (-13% in the 50 mg group) or LDL-C (-11% in the 150mg group). Patients with elevated baseline triglycerides (≥200 mg/dL; n=16) across all dose groups had a median reduction at day 28 from baseline of -24% (p <0.01).
At day 28, 43% of patients in all three dose groups showed ≥ 10% liver fat reduction from baseline as measured by magnetic resonance imaging – proton density fat fraction (MRI-PDFF). In this subgroup, there was a significant reduction from baseline in median liver fat content (-18%, -19%, and -23%, in the 50 mg, 150 mg and 600 mg groups respectively). The reduction of liver fat content was accompanied by a significant median reduction from baseline of serum ALT (-21%, -19%, and -32%, in the 50 mg, 150 mg and 600 mg groups respectively).
DUR-928 was well tolerated at all three doses evaluated. There were no serious adverse events reported during the study. Pharmacokinetic (PK) parameters after repeat dosing were comparable to those after a single dose (from a prior study), indicating no accumulation after repeat dosing. Drug exposure was dose dependent.
Results, including biomarker data, are still being analyzed.
“The results from this trial are encouraging given the short treatment course of 4 weeks to establish proof of concept,” stated Dr. Eric Lawitz,
“It is impressive to see these improvements after such a short treatment period,” stated
Topline Data Summary (Day 28 vs Baseline)
For all tables below, * Indicates p-value <0.05; ** indicates p < 0.01; *** indicates p <0.001
Clinical Chemistry |
|||
Median |
50 mg QD |
150 mg QD |
300 mg BID |
ALT |
-16%* (n=22) |
-10% (n=20) |
-17%*** (n=20) |
AST |
-14% (n=22) |
-9% (n=20) |
-18%** (n=20) |
GGT |
-6% (n=23) |
-1% (n=20) |
-8%* (n=21) |
LDL-C |
-6% (n=22) |
-11%* (n=20) |
-7% (n=21) |
Non-HDL-C |
-8% (n=23) |
-5% (n=20) |
-1% (n=21) |
Triglycerides |
-13%* (n=23) |
-3% (n=20) |
-2% (n=21) |
ALT (alanine aminotransferase); AST (aspartate aminotransferase); GGT (gamma-glutamyl transferase); LDL-C ( Low-Density Lipoprotein – Cholesterol); Non-HDL-C (Total cholesterol excluding High-Density Lipoprotein – Cholesterol); QD (once a day); BID (twice a day) |
Non-Invasive Imaging |
|||
Median |
50 mg QD |
150 mg QD |
300 mg BID |
MRI-PDFF |
-7% (n=21) |
-7% (n=21) |
-4% (n=21) |
Fibroscan |
-10%** (n=22) |
-9% (n=20) |
-1% (n=21) |
MRI-PDFF (Magnetic Resonance Imaging – Proton Density |
The following tables show Day 28 vs Baseline data from patients with ≥ 10% Reduction in MRI-PDFF
Clinical Chemistry Patients with ≥ 10% Reduction in MRI-PDFF |
|||
Median |
50 mg QD (n=9) |
150 mg QD (n=8) |
300 mg BID (n=9) |
ALT |
-21%** |
-19%* |
-32%*** |
AST |
-24%** |
-21% |
-39%*** |
GGT |
-13%*** |
-16%* |
-14% |
LDL-C |
-7% |
-11% |
-8%* |
Non-HDL-C |
-10% |
-8%* |
-12%* |
Triglycerides |
-9% |
0% |
-8% |
ALT (alanine aminotransferase); AST (aspartate aminotransferase); GGT (gamma-glutamyl transferase); LDL-C ( Low-Density Lipoprotein – Cholesterol); Non-HDL-C (Total cholesterol excluding High-Density Lipoprotein-Cholesterol); QD (once a day); BID (twice a day) |
Non-Invasive Imaging Patients with ≥ 10% Reduction in MRI-PDFF |
|||
Median |
50 mg QD (n=9) |
150 mg QD (n=9) |
300 mg BID (n=9) |
MRI-PDFF |
-18%*** |
-19%*** |
-23%*** |
Fibroscan |
-7% |
-9%** |
-9% |
MRI-PDFF (Magnetic Resonance Imaging – Proton Density |
About the Study
The study was a randomized, open label, multi center US study to evaluate safety, pharmacokinetics and signals of biological activity of DUR-928 in NASH patients with stage 1-3 fibrosis. A total of 65 patients completed the study. DUR-928 was orally administered daily at 50 mg (n=23), 150 mg (n=21), or 600 mg (300 mg BID (n=21)). Patients in this trial were dosed daily for 4 weeks and followed up for an additional 4 weeks.
About DUR-928
DUR‑928 is a new chemical entity and the first endogenous epigenetic regulator clinically tested for difficult-to-treat liver diseases. It is the lead candidate in
About
DURECT Forward-Looking Statement
The statements in this press release regarding the potential for DUR-928 to treat NASH patients and other plans for clinical development of DUR-928, including plans to conduct a Phase 2 clinical trial of DUR-928 in COVID-19 patients, and the potential benefits and uses of our drug candidates, including the potential use of DUR-928 to treat acute organ injuries such as AH and COVID-19 patients with acute liver or kidney injury, are forward-looking statements involving risks and uncertainties that can cause actual results to differ materially from those in such forward-looking statements. Potential risks and uncertainties include, but are not limited to, the risks that future clinical trials of DUR-928 do not confirm the results of trials conducted on small numbers of patients, are not started when anticipated, take longer to conduct than anticipated, do not generate similar positive results as generated in earlier clinical or pre-clinical trials, or do not demonstrate the safety or efficacy of DUR-928 in a statistically significant manner, the risk that the remaining data from the Phase 1b NASH trial reported in this press release is not consistent with the topline data reported here, the risk of disruptions to our business operations resulting from the COVID-19 pandemic, the risk that additional time and resources may be required for development, testing and regulatory approval of DUR-928, potential adverse effects arising from the testing or use of our drug candidates, our potential failure to maintain our collaborative agreements with third parties such as Gilead or consummate new collaborations and risks related to our ability to obtain capital to fund operations and expenses. Further information regarding these and other risks is included in
NOTE: POSIMIR® and SABER® are trademarks of
SOURCE
Corporate Contact, Mike Arenberg, DURECT, Chief Financial Officer, +1-408-346-1052, mike.arenberg@durect.com; Media Contact, Alison Chen, LifeSci Communications, +1-646-876-4932, achen@lifescicomms.com