Tuesday 3rd December – Day 1 Main ConferenceTuesday, 3 December 2024 - GMT (Greenwich Mean Time, GMTZ)

• The forgotten millions: overview of the immense unmet need facing the rare disease community.
• How investment fuels recent breakthroughs, especially within cell & gene therapy
• The necessity of partnerships between researchers, investors, the industry, and patient advocacy groups to transform healthcare for rare diseases.

NextCell Pharma is a clinical cell therapy company working in the autoimmune and inflammatory disease space. Their lead drug candidate, ProTrans is comprised of umbilical cord mesenchymal stromal cells (UC-MSC) selected using the company’s proprietary selection algorithm and pooled to generate the cryopreserved therapy. ProTrans has been used in Phase I and II trials for the treatment of type 1 diabetes and in severe lung hyperinflammation due to viral pneumonia.

Dr Davies is the Chief Scientific Officer for NextCell Pharma and will present the company’s current clinical portfolio for type 1 diabetes. The company has conducted a Phase I open label dose-escalation study with a primary endpoint of safety, as well as a Phase II double-blinded, randomised and placebo-controlled study with a primary endpoint of Δ-change in C-peptide area under the curve for a mixed meal tolerance test at 1 year following ProTrans/placebo infusion compared with baseline performance prior to treatment.

Dr Davies will share data demonstrating the efficacy of ProTrans treatment on preserving endogenous insulin production in newly diagnosed type 1 diabetes patients and the company’s long-term follow-up indicating that a single infusion of ProTrans results in a disease altering effect, with a slowing of disease progression for >3.5 years.

The company is now participating in a Phase II paediatric trial for the treatment of newly diagnosed diabetes in individuals aged 7-21. An update on the current trial status and vision for the future will be discussed as part of this presentation.

Practical solutions to achieve a 'get it right the first time' bioprocess, from the experience of running a multi-national, multi-product clinical cell therapy manufacturing portfolio. Early drug development decisions are critical to the commercialisation pathway, and understanding the healthcare landscape, treatment setting and infrastructure are necessary to design a competent CMC strategy for growth. However, drug manufacturing to meet the scale and agility necessary to support clinic-driven development is highly challenging. Real-world solutions to starting material selection, and technology intensification for downstream and fill finish solutions will be discussed to elucidate on building a successful CMC production strategy to meet patient demands and global supply. Manufacturing solutions to support early-through-late stage cell therapy clinical studies are not readily available, with a technological chasm occurring between early-phase 'academic' solutions and commercial-ready high capital unit operations. Here, practical solutions have been derived, and are in clinical GMP operations, for an off-the-shelf cell therapy portfolio to highlight development pathways for novel therapies within a small biotech company. Specifically, solutions to address batch-to-batch variability, to support patient demand and global supply, and to present a novel fill/finish scalable solution will be shown: all designed to bridge the technological chasm and provide bioprocessing throughout clinical development and beyond. Clinical success can be streamlined through value-driven early CMC decisions, with choices led by patient and clinic-led decisions. Drug development must be supported by a robust and agile bioprocess, with the solutions presented here aiming to bridge clinical phase production strategies.

In the rapidly evolving field of Cell and Gene Therapy (CGT), making strategic decisions early in the development cycle is crucial for ensuring long-term commercial success and delivering life-saving, affordable treatments to patients. This session will explore the critical importance of a phase-appropriate approach to commercial scale-up, highlighting key considerations including product dynamics, value chain design, capability mapping, and regional scaleout challenges.

Participants will gain insights into:

• Understanding the unique product dynamics of CGTs and their non-standard lifecycle.
• Designing robust value chains that adapt through each development phase.
• Mapping out capabilities required across different CGT modalities and strategically building these capabilities.
• Implementing new capabilities with prudence to avoid inefficiencies and added costs.
• Scaling modalities both individually and as part of an aggregated pipeline strategy.

Planning, strategic partnerships, and the integration of advanced technologies can ensure the successful commercialization of CGT products, maintaining quality, compliance, and timely delivery across global markets. Informed, timely decisions will drive the success of these transformative therapies.

Cytokine Release Syndrome (CRS) is a potentially life-threatening side effect associated with many modern immunotherapies such as CAR T cell therapy and T cell engaging bispecific antibodies. Despite incidence rates of up to 95% and significant escalation of medical costs very few treatment options are available, with only tociluzumab approved for CAR T cell induced CRS within the US. No preventative methods exist despite significant physician and patient needs. A range of investigational and repurposed drugs have been evaluated but have failed to produce sufficient reductions in CRS levels to impact patient management plans. A number of MAPK inhibitors have now been shown to enhance cell therapies and offer an ideal method to attenuate hypercytokinaemia associated with CRS without impairing immunotherapy efficacy. POLB 001 is an oral p38 MAPK inhibitor in development for the prevention of CRS. It has been evaluated in a Phase 1b LPS challenge study showing potency in dramatically reducing IL-6, TNFa, IL-8 and other proinflammatory cytokines along with meaningful reductions in heart rate, temperature and C-reactive protein increases. Phase 2 trials are planned with the intent to enable broader and safer uptake of immunotherapies in the clinic.

The advancement of allogeneic therapies presents a promising frontier in regenerative medicine, offering the potential for scalable, off-the-shelf treatments. However, the development of these therapies faces significant challenges, including the complexity of manufacturing processes and the need for consistent product quality. This abstract outline an approach to streamline allogeneic product development through the integration of platform automation in both 2D and 3D cell culture systems.

By leveraging automated platforms, Bayer aims to industrialize the efficiency and reproducibility of allogeneic cell production. Automation technology facilitates control over the cell culture environment, ensuring consistent cell quality and yield. In 2D systems, automation supports the standardization of monolayer cell cultures, while in 3D systems, it enables the scalable production of clusters or spheroids, which more closely mimic the in vivo cell environment.

The implementation of platform automation in allogeneic product development not only accelerates the production process but also reduces the risk of human error and variability. This approach promises to lower the barriers to entry for allogeneic therapies, making these innovative treatments more accessible to patients in need.

• Algorithms for optimization – how can AI predict optimal conditions to maximize yield and quality?
• Predictive analytics for cell growth, differentiation, and impurity forecasts to enhance process control
• Data-driven decision making
• How data analytics can help with heterogeneity of patient cells

• Regulatory frameworks for advanced therapies across key markets (FDA, EMA, MHRA)
• Handling the unique challenges and unknowns with advanced cell therapies
• Importance of long-term monitoring compared to previous biologics
• Accelerated Pathways
  • What expedited approval mechanisms are there (PRIME, RMAT etc.) impacting innovation