Even when despair medicine deal with identified and validated targets, their business potential might be constrained by dosing or security limitations. Seaport Therapeutics’ medicine use a novel supply method to beat these limitations. The startup launched on Tuesday, backed by $100 million in financing.
Boston-based Seaport was fashioned by PureTech Well being, an organization that creates startups, usually round a platform expertise. One notable instance is neuropsychiatric medicine developer Karuna Therapeutics, which grew and finally spun out of PureTech as a publicly traded firm with a lead drug taking a novel method to schizophrenia. Bristol Myers Squibb final yr struck a $14 billion deal to accumulate Karuna, whose schizophrenia drug is presently underneath FDA assessment.
Former Karuna CEO Steven Paul is chair of Seaport’s board of administrators. The startup’s expertise platform, Glyph, leverages the lymphatic system for drug supply. The corporate says its medicine are absorbed like dietary fat by means of the interior lymphatic system after which transported into circulation.
Glyph analysis was printed in 2021 within the Journal of Managed Launch and in 2022 in Frontiers in Pharmacology. The expertise was initially developed at Monash College in Australia. In 2017, PureTech licensed the platform, which it continued to develop in a subsidiary named Glyph Biosciences. That firm was later merged with different PureTech subsidiaries, which collectively produced a pipeline that features Seaport’s two most superior drug candidates.
Seaport’s SPT-300 is a prodrug, a substance that’s pharmacologically inactive till changing into an energetic therapeutic contained in the physique. SPT-300 is an oral prodrug of allopregnanolone, a neurosteroid discovered within the physique that regulates GABA-A receptors. Sage Therapeutics has already proven that these receptors might be efficiently drugged with Zulresso, the biotech’s FDA-approved post-partum despair drug. Whereas Zulresso is chemically equivalent allopregnanolone, it requires a burdensome 60-hour steady infusion.
Sage does have an oral various with Zurzuvae, a small molecule that additionally regulates GABA-A receptors. However FDA approval of Zurzuvae final yr lined solely post-partum despair, and never the a lot bigger main depressive dysfunction indication the corporate additionally sought. The regulator informed Sage extra medical testing is required to reveal effectiveness on this indication.
In accordance with Seaport, SPT-300 (referred to as LYT-300 throughout its improvement inside PureTech) retains the exercise and efficiency of endogenous allopregnanolone, however in an oral type that “has the potential to seize the breadth of the pure organic response.” The corporate added that this prodrug demonstrated proof-of-concept in a validated medical mannequin of tension in wholesome volunteers. The drug is presently in mid-stage improvement for treating main despair with anxiousness.
“We consider providing the confirmed mechanism of pure allopregnanolone by way of the modern orally administered method of LYT-300 represents an development that might have a really significant influence for sufferers,” PureTech CEO Daphne Zohar wrote in a letter to traders included within the firm’s 2022 annual report. “LYT-300 can also unlock the category of medicines focusing on GABA-A receptors, which has the potential to supply benefits over present requirements of care, corresponding to fast onset of motion, for a spread of situations together with despair, anxiousness, and others.”
Seaport says Glyph allows it to develop oral medicine with higher facet impact profiles. The expertise additionally circumvents excessive first-pass metabolism, wherein metabolism of a drug at a particular location within the physique reduces the quantity of energetic drug out there to succeed in circulation. That functionality is essential to the Seaport program SPT-320, a prodrug of agomelatine. Agomelatine medicine have been authorized as antidepressants in Europe and Australia, however not the U.S. Agomelatine is related to the next danger of liver harm attributable to excessive metabolism of the drug within the organ. Seaport says SPT-320 makes use of Glyph to bypass first-pass liver metabolism, which may in flip require decrease dosing and get rid of the necessity to monitor liver perform in sufferers. This Seaport program is in preclinical improvement for generalized anxiousness dysfunction.
A 3rd Seaport program, SPT-348, is a prodrug of a non-hallucinogenic neuroplastogen. This discovery-stage analysis may result in a brand new therapy for temper and different neuropsychiatric problems. SPT-348 leverages Glyph to enhance sure properties, corresponding to how the drug interacts with the physique in addition to its tolerability. Different packages in discovery and preclinical improvement deal with targets that stay undisclosed.
“Given the traditionally low success charges inside neuropsychiatric drug improvement, exactly fixing the earlier limitations of clinically validated mechanisms improves the chance of success and allows us to considerably speed up improvement,” Paul, who was additionally a Sage co-founder, mentioned in a ready assertion.
Seaport’s Sequence A financing was co-led by Arch Enterprise Companions and Sofinnova Investments together with Third Rock Ventures and PureTech Well being. Together with the financing, Seaport introduced the appointment of Zohar as Seaport CEO and board member.
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