Therapeutics

AR1001

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Overview

Name: AR1001
Therapy Type: Small Molecule (timeline)
Target Type: Other (timeline)
Condition(s): Alzheimer's Disease
U.S. FDA Status: Alzheimer's Disease (Phase 3)
Company: Aribio Co., Ltd.

Background

Ar1001 is a selective inhibitor of phosphodiesterase 5. This new pyrrolo-pyrimidinone was first developed for treatment of erectile dysfunction in South Korea, and is now being tested for Alzheimer’s disease. Its maker claims AR1001 to be 10-fold more potent at inhibiting PDE5, and better at entering the brain, than approved PDE5 inhibitors, including sildenafil.

The rationale for using PDE5 inhibitors in AD stems from animal studies, where these compounds enhance memory and learning by increasing the intracellular messenger cGMP, and also possibly by improving blood supply to the brain. Several PDE5 inhibitors have been reported to curtail amyloid production, and to lessen neuroinflammation and learning and memory deficits in mouse models of AD (see review by Zuccarello et al., 2020).

Three studies have reported PDE5 effects in people. Men being treated for erectile dysfunction with low doses of the PDE5 inhibitors tadalafil or udenafil daily for eight weeks improved performance on tests of cognition and cerebral blood flow, while a single dose of sildenafil improved brain blood supply in people with AD (Choi et al., 2019; Shim et al., 2014Sheng et al., 2017). A study of potential AD targets for drug repurposing has identified sildenafil, and a medical records analysis reported that men who used it lowered their risk of AD by 69 percent (Fang et al. 2021). Other analyses found no such evidence (Desai et al., 2022)

The only public preclinical data on AR1001 was presented by Aribio at AAIC 2020, where the company reported reduced Aβ plaque deposition in 5XFAD mice, and improved memory in NSE/APP-C105 mice after treatment (Kang et al., 2020). The company later published similar results using the approved PDE5 inhibitor mirodenafil (Kang et al., 2022).

Findings

In April 2019, Aribio began a Phase 2 study of efficacy in clinically diagnosed people with mild to moderate AD. The trial recruited 210 subjects at 21 sites in the U.S. A 26-week course of 10 or 30 mg daily AR1001 or placebo was followed by an optional 26-week extension, where the 10 and 30 mg groups continued at that dose, and placebo takers were randomized to 10 or 30 mg. Primary endpoints were change from baseline in ADAS-Cog13 and ADCS-CGIC; secondary endpoints included various measures of cognition, behavior and function, and exploratory plasma biomarkers. The study ended in June 2021, and results were presented at the CTAD conference in November. There was no significant change from baseline in either the ADAS-Cog13 or ADCS-CGIC at 26 or 52 weeks, and no difference from placebo at 26 weeks.

More than half of participants were taking other, unspecified AD medications, and a post hoc subgroup analysis hinted those taking 30 mg AR1001 alone, but not those with concomitant treatment, might have improved on the ADAS-Cog13. The mild, but not the moderate, subgroup also showed improvement on the same endpoint. There was no placebo group for comparison at 52 weeks. The treatment was well-tolerated, with a similar incidence of side effects and discontinuation in all groups. There was one death from COVID, and one person on the high dose had a serious adverse event of fainting, possibly related to drug. According to additional data presented at the October 2023 CTAD conference, both doses led to a decrease in plasma pTau181, compared to an increase in the placebo group. A post hoc analysis suggested that in people with the highest pTau181 levels at the start, and thus most likely to be amyloid positive, the 30 mg dose may have slowed decline on the ADAS-Cog13.

In December 2022, the company began a Phase 3 study in people with MCI or mild dementia due to AD. Called Polaris-AD, it is enrolling, at approximately 65 research sites, 1,150 people with MMSE scores above 20, CDR global ratings of 0.5 or 1, and RBANS of 85 or less, and confirmation of amyloid pathology by CSF test or PET. Participants will take one 30 mg tablet or placebo daily for one year. The primary outcome is change in the CDR-SB after one year; secondary outcomes include ADAS-Cog 13, the Amsterdam Instrumental Activities of Daily Living, Geriatric Depression Scale, MMSE, and RBANS. The study will also track safety, as well as plasma and CSF biomarkers, and offers a two-year open label extension. Completion is anticipated in December 2025.

Aribio has FDA approval for a Phase 2 trial in vascular dementia (Korea Biomedical Review news). On its pipeline, it also lists Phase 2 development for dementia with Lewy bodies and dementia with depression/PTSD, but no trials appear in common registries for these indications.

For details on AR1001 trials, see clinicaltrials.gov.

Last Updated: 19 Dec 2023

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References

Paper Citations

  1. Zuccarello E, Acquarone E, Calcagno E, Argyrousi EK, Deng SX, Landry DW, Arancio O, Fiorito J. Development of novel phosphodiesterase 5 inhibitors for the therapy of Alzheimer's disease. Biochem Pharmacol. 2020 Jun;176:113818. Epub 2020 Jan 21 PubMed.
  2. Choi JB, Cho KJ, Kim JC, Kim CH, Chung YA, Jeong HS, Shim YS, Koh JS. The Effect of Daily Low Dose Tadalafil on Cerebral Perfusion and Cognition in Patients with Erectile Dysfunction and Mild Cognitive Impairment. Clin Psychopharmacol Neurosci. 2019 Aug 31;17(3):432-437. PubMed.
  3. Shim YS, Pae CU, Cho KJ, Kim SW, Kim JC, Koh JS. Effects of daily low-dose treatment with phosphodiesterase type 5 inhibitor on cognition, depression, somatization and erectile function in patients with erectile dysfunction: a double-blind, placebo-controlled study. Int J Impot Res. 2014 Mar-Apr;26(2):76-80. Epub 2013 Nov 28 PubMed.
  4. Sheng M, Lu H, Liu P, Li Y, Ravi H, Peng SL, Diaz-Arrastia R, Devous MD, Womack KB. Sildenafil Improves Vascular and Metabolic Function in Patients with Alzheimer's Disease. J Alzheimers Dis. 2017;60(4):1351-1364. PubMed.
  5. Fang J, Zhang P, Zhou Y, Chiang CW, Tan J, Hou Y, Stauffer S, Li L, Pieper AA, Cummings J, Cheng F. Endophenotype-based in silico network medicine discovery combined with insurance record data mining identifies sildenafil as a candidate drug for Alzheimer’s disease. Nat Aging. 1, 2021, pp. 1175–88. Nat Aging.
  6. Desai RJ, Mahesri M, Lee SB, Varma VR, Loeffler T, Schilcher I, Gerhard T, Segal JB, Ritchey ME, Horton DB, Kim SC, Schneeweiss S, Thambisetty M. No association between initiation of phosphodiesterase-5 inhibitors and risk of incident Alzheimer's disease and related dementia: results from the Drug Repurposing for Effective Alzheimer's Medicines study. Brain Commun. 2022;4(5):fcac247. Epub 2022 Oct 4 PubMed.
  7. Kang BW, Kim F, Choi YP, Lee Y, Kwak DE, Shin J, Kim YS, Choung JJ, Rhee J. AR1001 ameliorates Alzheimer’s disease pathology and symptoms by multi-mechanisms. Alzheimer's & Dementia, 07 December 2020
  8. Kang BW, Kim F, Cho JY, Kim S, Rhee J, Choung JJ. Phosphodiesterase 5 inhibitor mirodenafil ameliorates Alzheimer-like pathology and symptoms by multimodal actions. Alzheimers Res Ther. 2022 Jul 8;14(1):92. PubMed.

External Citations

  1. Korea Biomedical Review news
  2. pipeline
  3. clinicaltrials.gov

Further Reading

Papers

  1. Samudra N, Motes M, Lu H, Sheng M, Diaz-Arrastia R, Devous M, Hart J, Womack KB. A Pilot Study of Changes in Medial Temporal Lobe Fractional Amplitude of Low Frequency Fluctuations after Sildenafil Administration in Patients with Alzheimer's Disease. J Alzheimers Dis. 2019;70(1):163-170. PubMed.
  2. Samidurai A, Xi L, Das A, Kukreja RC. Beyond Erectile Dysfunction: cGMP-Specific Phosphodiesterase 5 Inhibitors for Other Clinical Disorders. Annu Rev Pharmacol Toxicol. 2023 Jan 20;63:585-615. Epub 2022 Oct 7 PubMed.
  3. Chowdari Gurram P, Satarker S, Kumar G, Begum F, Mehta C, Nayak U, Mudgal J, Arora D, Nampoothiri M. Avanafil mediated dual inhibition of IKKβ and TNFR1 in an experimental paradigm of Alzheimer's disease: in silico and in vivo approach. J Biomol Struct Dyn. 2022 Dec 19;:1-19. PubMed.
  4. Phosphodiesterase-5 inhibitors for Alzheimer's disease?. Med Lett Drugs Ther. 2022 Oct 31;64(1662):174-175. PubMed.
  5. Pauls MM, Binnie LR, Benjamin P, Betteridge S, Clarke B, Dhillon MK, Ghatala R, Hainsworth FA, Howe FA, Khan U, Kruuse C, Madigan JB, Moynihan B, Patel B, Pereira AC, Rostrup E, Shtaya AB, Spilling CA, Trippier S, Williams R, Young R, Barrick TR, Isaacs JD, Hainsworth AH. The PASTIS trial: Testing tadalafil for possible use in vascular cognitive impairment. Alzheimers Dement. 2022 Dec;18(12):2393-2402. Epub 2022 Feb 8 PubMed.
  6. Hasan N, Zameer S, Najmi AK, Parvez S, Yar MS, Akhtar M. Roflumilast and tadalafil improve learning and memory deficits in intracerebroventricular Aβ1-42 rat model of Alzheimer's disease through modulations of hippocampal cAMP/cGMP/BDNF signaling pathway. Pharmacol Rep. 2021 Oct;73(5):1287-1302. Epub 2021 Apr 15 PubMed. RETRACTED
  7. Salem MA, Budzyńska B, Kowalczyk J, El Sayed NS, Mansour SM. Tadalafil and bergapten mitigate streptozotocin-induced sporadic Alzheimer's disease in mice via modulating neuroinflammation, PI3K/Akt, Wnt/β-catenin, AMPK/mTOR signaling pathways. Toxicol Appl Pharmacol. 2021 Oct 15;429:115697. Epub 2021 Aug 21 PubMed.
  8. Newby D. Are phosphodiesterase Type 5 inhibitors potential therapies for Alzheimer's disease and related dementias?. Brain Commun. 2022;4(5):fcac260. Epub 2022 Oct 11 PubMed.