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Novel Treatment for Gout and Hyperuricemia

Intra-articular injections of modified hyaluronic acid significantly reduces inflammation-induced swelling in gout

X-ray of foot
Please note image is purely illustrative. Source: Hellerhoff, Wikimedia, CC BY-SA 3.0

Background

Hyperuricemia (HA), elevated serum urate levels, is a major risk factor for gout, the major form of arthritis globally. It is estimated to affect approx. 3.9% of adults in the United States (8.3 million). Old drugs are current gold standards (colchicine, allopurinol) and many have adverse side effects with black-box warning labels - drug compliance is poor. There are two main classes of drugs: urate synthesis inbibitors (USI) - drugs that prevent uric acid production by xanthine oxidase (XO); or drugs that enhance renal excretion by inhibiting reabsorption (uricosurics). Uricosurics in particular have safety issues.

Chronic gout guidelines recommend lowering UA levels by the use of USI, such as allopurinol or Uloric (febuxostat), as the first-line treatment. However, inability to achieve target UA levels with USI has led to co-treatment or combination drug development with uricosurics. Finally, for the treatment of refractory gout an injectable drug, Kytrexxa (pegylated uricase) is used to actively transform uric acid into a more readily excretable form, allantoin. Kytrexxa use is limited by severe safety limitations: black box warning for anaphylaxis and infusion reactions (up to 90% patients have antibody response) and is contraindicated in patients with G6PD deficiency. Thus there remains a significant unmet need for safe and efficacious treatments in both hyperuricemia and gout.

Technology Overview

HA has unique biophysical properties making it valuable in a number of existing products. However a major limitation in vivo is that HMW HA degrades into LMW forms which are proinflammatory by activating Toll-like Receptor-4 (TLR4). Researchers at Queen鈥檚 University have now identified novel N-acyl analogs of HA, in particular N-butyl HA (BHA), which prevent LMW HA from activating TLR4 and the inflammasome 鈥 a key mechanism involved in the pathogenesis of hyperuricemia and gout. Hyperuricemia is also associated with oxidative stress due to production of reactive oxygen species (ROS) from increased XO expression and activity. Such species result in degradation of HMW HA producing LMW HA and further activating TLR4 and inflammasome. Finally, urate itself is an activator of the inflammasome via TLR4 further supporting the potential benefit of this novel HA analogs in treating hyperuricemia.

Graph showing BHA effectiveness in gout model

The potential benefit of BHA in treating hyperuricemia and gout has been borne out in preclinical models. TLR4 has be demonstrated to be essential for the mouse gout model induced by urate monohydrate injection into joints. Thus the researchers chose this model as a first test for in vivo activity of BHA. In this model, a single 10 碌g or 50 碌g injection of BHA was given into joints of mice concomitantly with the monosodium urate. These treatments were compared to a current standard clinical treatment, colchicine, which was given prior to inducing the gout as well as after. In this model (Figure 1.) BHA significantly reduced inflammation-induced swelling to control levels (controls received saline injection) and BHA reduced swelling more quickly and to a larger extent than colchicine. Concurrent with these benefits significant beneficial changes were seen in serums levels of Il-1尾, IL-8, Il-10, MCP-1 and IFN纬. 

Graph showing uric acid reduction by BHA

Furthermore, in a hyperuricemia rat model a short term treatment of BHA given intraperitoneally significantly reduced serum uric acid as did oral allopurinol. Similarly BHA significantly reduced creatinine and urea nitrogen in liver and serum, significantly reduced XO activity in liver, and significantly reduced ROS levels in serum and liver. 

Stage of Development

Preclinical Development.

Further Deatils

See initial publication on mechanism of BHA and TLR4: Babasola O et al. Chemically modified N-acylated hyaluronan fragments modulate proinflammatory cytokine production by stimulated human macrophages. J Biol Chem. 2014 Sep 5;289(36):24779-91. 

Benefits

  • Short-term, non-optimized treatment with BHA provided significant efficacy to both hyperuricemia and gout as well as existing clinically used treatments. 
  • BHA is based upon HA and is highly likely to not have the negative limiting side-effects of existing treatments
  • Intra-articular injections already commonplace in gout

Applications

  • Treatment of hyperuricemia and gouty and likely expansion to nonalcoholic fatty liver disease (NAFLD) and nonalcoholic steatohepatitis (NASH)
  • Broad opportunity: other possible treatments included osteoarthritis (large existing injectable market), cosmeceuticals, COPD and ophthalmology 

Opportunity

Seeking exclusive licensee, venture funding or research collaborator 

Patents

  • Granted US Patents US 9,644,040, US 10,239,962 鈥淗yaluronic Acid Derivatives鈥
  • Granted Japanese Patent JP6363119 鈥淗yaluronic Acid Derivatives鈥
  • Granted Canadian Patent CA2905610 鈥淗yaluronic Acid Derivatives鈥
  • Granted US Patent US 11679123 鈥淣-Acetylated Hyaluronic Acids for Hyperuricemia and Gouty Arthritis鈥
  • Patent pending for wound healing and gouty arthritis in US, China and Canada

IP Status

  • Patented
  • Provisional patent

Seeking

  • Development partner 
  • Licensing
  • Seeking investment

Posted/updated

October 4, 2018 / September 20, 2023 (updated patents)