By Delilah Alvarado
Published July 14, 2026
In a significant vote of confidence for the resurgence of psychiatric drug development, U.K.-based biotech firm Draig Therapeutics announced on Tuesday the successful closure of a $65 million Series B financing round. The capital infusion is earmarked to accelerate the clinical evaluation of the company’s lead experimental candidate, DT-101, which aims to reshape the treatment landscape for major depressive disorder (MDD) and other complex psychiatric conditions.
The round was spearheaded by Deep Track Capital, a prominent investor in the life sciences sector, with substantial participation from industry heavyweights including Janus Henderson Investors and Marshall Wace. This latest financial milestone brings Draig’s total funding to over $200 million since the company emerged from stealth operations just last year, marking it as one of the most closely watched entities in the neuroscience space.
The Core Objective: Targeting Brain Chemistry
Draig Therapeutics, a spin-out from the rigorous research environment of Cardiff University in Wales, was founded on the premise that current psychiatric treatments often fail because they lack precision. The company’s therapeutic philosophy centers on correcting fundamental chemical imbalances in the brain—specifically, restoring the equilibrium between "excitatory" and "inhibitory" signaling pathways.
At the heart of the company’s pipeline is DT-101, a small-molecule candidate that targets AMPA receptors. In individuals suffering from major depressive disorder, these receptors are frequently compromised, leading to a breakdown in neural communication. By modulating these receptors, Draig believes it can stabilize brain activity, offering a potential "best-in-disease" efficacy profile that goes beyond the symptomatic relief provided by traditional antidepressants.

"Our mission is to move past mere management of symptoms," said Draig CEO Ivana Magovčević-Liebisch in an email to BioPharma Dive. "The goal is to restore the brain to a healthier state and enable patients to live their best lives. This funding provides us with the runway to prove that our scientific approach can translate into meaningful, durable outcomes for patients who have exhausted current treatment options."
Chronology: From Academic Spin-out to Clinical Pivot
The trajectory of Draig Therapeutics reflects a rapid maturation process typical of high-potential biotech startups.
- Pre-2025: Foundational research is conducted at Cardiff University, focusing on the neurobiology of AMPA and GABA-A receptors.
- July 2025: Draig emerges from stealth mode, securing a massive $140 million Series A round. The company introduces its core platform and a trio of initial drug candidates.
- Late 2025 – Early 2026: The company initiates a global Phase 2 study of DT-101 as a monotherapy and begins a parallel U.S.-based trial testing the drug as an adjunctive treatment alongside existing therapies.
- July 14, 2026: Draig closes a $65 million Series B round, reinforcing its balance sheet ahead of anticipated data readouts.
According to Magovčević-Liebisch, the company was already well-capitalized prior to this latest round. The decision to raise additional funds now—rather than waiting—is a strategic move to accelerate the timeline for its clinical trials and broaden the scope of its secondary programs, which focus on GABA-A receptor modulation.
The High-Stakes Landscape of Psychiatric Research
Psychiatry has historically been viewed as a "graveyard" for pharmaceutical innovation. The inherent complexity of the human brain, combined with the difficulty of defining clinical endpoints for subjective disorders, has led to a long string of high-profile failures. For decades, many large pharmaceutical companies retreated from neuroscience, viewing the risk-to-reward ratio as unfavorable compared to oncology or rare diseases.
However, the narrative is shifting. Recent breakthroughs in neuroscience have reignited investor interest, proving that with the right target selection, significant value can be unlocked. The acquisition of Karuna Therapeutics by Bristol Myers Squibb for its schizophrenia program served as a watershed moment, signaling that big pharma is once again hungry for late-stage psychiatric assets.

Draig is positioning itself to capitalize on this renewed momentum. By focusing on well-validated but difficult-to-drug targets like AMPA and GABA-A receptors, the company is bridging the gap between historical neurobiology and modern, precision-based drug discovery.
Supporting Data and Technical Rationale
The scientific rationale behind DT-101 is supported by a growing body of evidence suggesting that glutamate signaling—mediated by AMPA receptors—is a key driver of depressive symptoms. Traditional treatments, such as Selective Serotonin Reuptake Inhibitors (SSRIs), primarily target monoamine pathways, which can take weeks to show efficacy and often result in incomplete remission.
Draig’s approach aims for a more rapid and robust intervention. By modulating the excitatory/inhibitory balance, the company hopes to address the neuroplasticity deficits that characterize chronic depression.
While the company has not yet published its full Phase 2 data, the "real conviction" mentioned by leadership stems from early-stage clinical signals. These signals have emboldened the company to pursue a dual-track development strategy:
- Monotherapy trials: Assessing DT-101’s ability to stand alone as a primary treatment.
- Adjunctive trials: Testing the drug’s potential to boost the efficacy of standard-of-care treatments, providing a faster path to market for patients who remain treatment-resistant.
Strategic Implications: What Comes Next?
The $65 million injection serves a dual purpose: it provides the financial security to survive the "valley of death" between Phase 2 and Phase 3 trials, and it allows for the parallel development of Draig’s secondary candidates. While the company has been tight-lipped regarding the specific indications for its GABA-A receptor programs, their inclusion in the pipeline suggests a broader ambition to tackle a range of neuropsychiatric conditions beyond MDD, potentially including anxiety disorders or treatment-resistant bipolar disorder.

The broader implications for the biotech sector are equally notable. This deal suggests that private equity and venture capital firms remain bullish on "platform-based" neuro-biotech. Investors are increasingly looking for companies that have moved past the "concept" stage and are actively generating clinical data.
For the patients, the promise of a "best-in-disease" treatment remains the ultimate prize. If DT-101 delivers on its clinical potential, it could provide a much-needed alternative in a market that has seen little in the way of truly novel mechanisms of action over the last decade.
Conclusion
As Draig Therapeutics moves forward with its current trials, the industry will be watching closely. The success of the Series B round serves as a testament to both the strength of the company’s underlying science and the renewed appetite for innovation in mental health.
With significant funding now secured and a clear development roadmap, Draig is firmly positioned to test whether its "best-in-disease" hypothesis can survive the scrutiny of large-scale clinical trials. Should the company’s data readouts in the coming year reflect the optimism of its investors, Draig may well find itself at the center of the next great wave of psychiatric drug innovation—a transition that would be welcomed by clinicians and patients alike.
As Magovčević-Liebisch noted, the goal is simple but profound: to change the lives of millions by understanding the brain’s delicate, but repairable, machinery. With this latest round of funding, that goal is now one significant step closer to reality.
