%prioritycode% Allogeneic and Autologous Cell Therapies Report 2022

This full report by Informa Connect and Catalent reveals emerging trends in allogeneic and autologous cell therapy space.

Allogeneic and Autologous Cell Therapies Report 2022

Product types, manufacturing strategies and future trends across the industry

INTRODUCTION

In December 2021, Informa Connect and Catalent conducted a worldwide survey of cell therapy professionals to understand the emerging trends in both the allogeneic and autologous cell therapy space.

Respondents were asked about their focus areas, product types and phases of their programs, in addition to their decision-making and the most significant challenges to their manufacturing goals.

The full report reveals cell therapy manufacturing trends amid the rapid progression of cell therapy technologies.

KEY FINDINGS INCLUDE:

63% of cell therapy professionals are working on both autologous and allogeneic products

Supply chain bottlenecks are the most common hurdle that cell therapy professionals have experienced with their programs

Respondents gave valuable insights into next-generation innovative technologies they are most likely to adopt

About Catalent

Catalent Cell & Gene Therapy is an industry-leading technology, development, and manufacturing partner for advanced therapeutics. Its comprehensive cell therapy portfolio includes a wide range of expertise across a variety of cell types including CAR-T, TCR, TILs, NKs, iPSCs, and MSCs.

With deep expertise in viral vector development, scale-up and manufacturing for gene therapies and viral vaccines, Catalent is a full-service partner for plasmid DNA, adeno-associated viral (AAV), lentiviral and other viral vectors, and oncolytic viruses.

An experienced and innovative partner, it has a global network of dedicated, small- and large-scale clinical and commercial manufacturing facilities, including an EMA- and FDA-licensed viral vector facility, and fill/finish capabilities located in the U.S. and Europe.

With integrated solutions for plasmid DNA, viral vectors and autologous and allogeneic cell therapies through clinical trial packaging and logistics, Catalent can provide full supply chain control, helping innovators get their advanced therapies to patients, faster.

Demographics

Organizations, job functions and regions

DEMOGRAPHICS

44% of the respondents indicate they are from biotech, while the remainder show an even distribution across service providers, pharmaceutical companies and academia.

44% of the respondents hold senior-level roles such as VP, Head or Director, while scientists emerge as the next largest section of the respondents. Combined with the other job function categories, the respondents reflect a strategic mix which is critical for driving innovation in the cell therapy space.

More than half of the respondents reside in North America, while just less than a third are based in Europe, key investment geographies for cell and gene therapy.

Product types

Therapy focus areas, types and product pipelines

PRODUCT TYPES

More than half of the respondents work in companies with a focus on oncology, and 1 in 4 respondents work in companies with a focus on cardiovascular or autoimmune disorders.

63% of the respondents say they are working on both autologous and allogeneic products, however allogeneic products are the most popular cell therapy type.

More than half of respondents have cell therapy clinical trials in their preclinical or phase I stage, while a third are running trials in either discovery or phase II.

More than half of the respondents say their companies have gene-enabled cell therapies such as CAR-T and CAR-NK in their production pipeline.

Another 42% indicate that their companies are focusing on non-modified cell therapies such as MSCs and TILs, and just under 1 in 3 report that their companies are working on production of iPSC-based cell therapies.

57% of respondents who are developing gene-edited cell therapies say that they are carrying out their viral vector and cell therapy manufacturing with the same partner.

38% of respondents who are developing non-modified cell therapies say that their cell type did not require gene editing for the disease their programs are focused on.

1 in 4 said that they chose their product type to simplify supply chain processes.

56% of respondents who are focused on iPSCs say that their companies are developing their own custom bank, while 44% say that they are using a commercially available iPSC GMP bank.

Manufacturing

In-house vs. outsourcing and the decisions behind it

MANUFACTURING

57.5% of respondents are manufacturing their cell therapy programs in-house, while 42.5% are manufacturing cell therapies with a partner.

57% of respondents who chose to manufacture in-house say that it was because they valued having better supply chain control.

53% of respondents who chose to outsource manufacturing say they did so due to a lack of in-house capacity, while just under a third say that it was to seek external manufacturing expertise.

<small>Challenges and Innovations</small>

Major hurdles, novel technologies and innovating autologous therapies

CHALLENGES AND INNOVATIONS

MAJOR HURDLES

What are the biggest bottlenecks or hurdles that you have experienced with your cell therapy program?

Top 3 Responses:

Supply Chain
Manufacturing and CDMOs
Finances & Cost

Supply chain bottlenecks are the most common hurdle that cell therapy professionals have experienced with their programs.

Selected responses:

"Speed of pre-clinical development and regulatory considerations"

"Getting into the queue for having plasmids and vectors produced"

"The challenges of working with an outside party to schedule and facilitate improvements to our manufacturing process"

"Manufacturing site planning, build-out, and qualification"

ADOPTING TECHNOLOGIES

Which next generation cell or gene therapy innovations or technologies are you likely to adopt?

Top 3 Responses:

Gene editing/CRISPR
Automated process systems
iPSCs

In response to this open question, gene editing and CRISPR technologies is the top innovation that respondents say that their companies are most likely to adopt. Automated process systems are the next most popular suggestion.

Selected responses:

"Migration to full automation"

"Allogeneic MSCs and possibly iPS cells for dogs"

"Non-viral gene editing"

"Online monitoring and rapid testing"

"Acoustofluidic technologies in the bioprocessing"

"CRISPR/Cas9"

62% of respondents say they are definitely likely to develop their autologous cell therapy program to support a bedside setting.

Allogeneic T-cell Therapies:

Efficient Commercial Manufacturing Readiness using “Manufacturing by Design” Methodology

ALLOGENEIC T-CELL THERAPIES: Efficient Commercial Manufacturing Readiness using “Manufacturing by Design” Methodology

The ex-vivo Cell and Gene Therapy medicine field has entered into a new era driven by the registration of the first autologous products namely Kymriah (Novartis, 2017, US), Yescarta (Kite/Gilead, 2017, US) and Strimvelis (GSK/Orchard, 2016, Europe).

Despite this very promising context, cell-based processes are far from being mature from an industrial perspective. One proof is the frequent news of quality issues (Out-of-Specification) on cell therapy products.

The industry overall has a driving need to develop “next-generation” autologous processes with the objective of improving manufacturability (process length, automation et al.) and to become increasingly commercially competitive.

Following closely behind the recent success of autologous cellular therapies, allogeneic T-cell therapies are moving toward late-stage clinical trials and commercial registration with the promise of having these breakthrough therapies available for market launch.

Consequently, a new race to market has begun among “allogeneic CAR-T pioneers” (e.g. Servier, Cellectis, Allogene, Crispr Therapeutics, Precision Bioscience et. al.).

Cell and Gene Therapy companies need to invest time, effort and funds to improve process manufacturability as it will be the key for long-term commercial success.

T-Cell-based products can be classified as non-traditional therapeutic products in the biotechnology industry and rely on complex and challenging process optimization and manufacturing.

The most common traits of both allogeneic and autologous processes are:

HIGH VARIABILITY due to the nature of the starting material (e.g. variety of cell types, living biological organisms). Non-industrial equipment that is often only partially compatible with current GMP standards

PROCESS SCALE with process volume ranging from a few millimeters to a few liters

ASEPTIC PROCESSING with no possibility to perform sterile filtration that is especially challenging for autologous production processes.

Contract development and manufacturing organizations need to play a critical role in the scale-up and industrialization of cellular therapies by providing customized tools and processes.

The Manufacturing by Design approach for addressing the industrialization of cell therapies allows for optimal production conditions.

Quality by Design

Quality by Design (QbD) methodology today is widely implemented by biopharmaceutical manufacturers following its widespread adoption in the field of small molecule active pharmaceutical ingredients (APIs).

In 2006, the International Conference on Harmonization presented QbD methodology that was later recommended by the Food and Drug Administration (FDA) as a systematic approach to process and product management with scientific risk assessment.

Catalent’s Cell Therapy team was an early adopter of QbD Methodology in the field of T-cell-based therapies.

Custom technology and service providers, like Catalent, work with innovators on defining the Quality Target Product Profile (QTPP), identifying Critical Quality Attributes (CQAs), and categorizing the Critical Process Parameters (CPPs), with the final goal of establishing a design space (FIGURE 1) and its associated control strategy.

FIGURE 1 Example of 3D design space visualization

QbD provides a solid foundation to improve process and product understanding but presents two limitations:

By definition, QbD is mainly focused on product quality. Other industrial considerations, such as process efficiency, are less frequently captured through this methodology. An attempt to extend the QbD approach to process efficiency and manufacturability was done in the A-VAX¹ case study in the chapter related to applying QbD to Live Vaccines. In the proposed approach, Key Process Attributes (KPA) are defined along with the classical CQA. A typical KPA could be the upstream process yield or the overall process output.
This approach is mainly applied to the Drug Substance and less to the Drug Product.

REFERENCES

1. A-VAX: Applying Quality by Design to Vaccines CMC-Vaccines Working Group May 2012: https://www.dcvmn.org/IMG/pdf/a-vax-applying-qbd-tovaccines_2012.pdf

Our Approach

From an industrial perspective and taking into consideration the current development status of cell-based products, the need to integrate the aspects of process performance and economics along with an end-to-end vision of the manufacturing process was identified.

Catalent’s Cell Therapy team internally developed a rationale-based methodology to address T-cell manufacturing challenges based on the intended final manufacturing process. This methodology is called Manufacturing by Design (MbD) and uses a similar approach as QbD for its implementation. TABLE 1 shows the terminology comparison of the two approaches.

TABLE 1: QbD vs. MbD

As previously mentioned, and as illustrated by FIGURE 2, MbD is intended to optimize:

PROCESS EFFICIENCY such as process robustness, process scalability and operability, supported by the definition of Critical Manufacturing Attribute (CMfAs)

ECONOMICS with Cost of Goods (CoGs) and business continuity

END-TO-END VISION from the starting material up to the final Drug Product including supply chain management

FIGURE 2 Focus areas of MbD

Manufacturing by Design

GENERIC ALLOGENEIC PROCESS

For the first roll-out of this approach, a case study with a generic allogeneic process illustrated in FIGURE 3 was used. The process steps considered are cell acquisition, preparation/selection, activation, electroporation and transduction, expansion, purification and formulation, fill and finish.

FIGURE 3 Typical process steps in a generic allogeneic T-cell therapy manufacturing process.

METHODOLOGY OVERVIEW

The MbD methodology was established after a series of internal workshops and similar tools (risk assessments, process analysis) as found in the QbD methodology. The different steps selected for the MbD methodology are summarized in FIGURE 4 (below).

FIGURE 4 MbD methodology overview

MAPPING OF MANUFACTURING CHALLENGES

As a critical starting point, all current manufacturing challenges were classified and mapped (FIGURE 5). The map includes a detailed mix of manufacturing attributes (scale-up, cost of goods), process steps (fill and finish, quality control) and industrial challenges (supply chain, manufacturing strategy).

FIGURE 5 Map of T-cell-based processes manufacturing challenges

SELECTION OF MANUFACTURING ATTRIBUTES AND PROCESS HEAT MAP

For this process, the definition of "Manufacturing Attribute" (MfA) was extended to cover industrial process designs that can impact the production process. Taking into account the attribute map in FIGURE 5, the final methodology was consolidated to include:

Processability
Manufacturing Strategy
Product Characterization
Cost of Goods
Raw Materials
Supply Chain

While the interpretation of several MfAs is relatively straight-forward (Cost of Goods, Raw Materials), others can be more complex to define such as “Processability” which covers process scalability and process operability including automation and system closure.

Another series of workshops were carried out to analyze how selected MfAs impact each process step, and ranking was achieved according to the impact level.

After several rounds of iteration, a process Heat Map was generated (FIGURE 6) with a level of criticality illustrated by a color code (from low criticality in green to high criticality in dark red).

The result was quite overwhelming as most of the Heat Map intersections were red. Therefore, we decided to focus on the dark-red intersections which represent about 40% of the Heat Map.

FIGURE 6 Process Heat Map. Process steps are listed and for each MfA, a color coding based approach was used to define criticality. This approach can be implemented to prioritize MfA and process steps for investigation.

From a quick analysis of this process Heat Map, the following conclusion can be drawn: the most critical process steps from a manufacturing point of view for an allogeneic process are the cell engineering (more precisely the cell transduction) and the fill and finish steps. On the other axis, the most critical MfAs are Processability, the cost of goods and the raw materials.

All of these critical intersections were further analyzed individually in order to understand the drivers of their criticality, the potential solutions needed to mitigate these issues and the feasibility to implement these solutions.

In order to prioritize internal process and technical development efforts
to overcome the current allogeneic process limitation, an impact
mapping approach was used based on the following criteria:

Impact based on the level of criticality of the topic analyzed
Difficulty of implementation based on the existence of a technical solution, the time and cost of implementation
Probability of success of solving the identified issues

FIGURE 7 shown opposite illustrates an extract (for readability consideration) of the outcome of this impact analysis.

FIGURE 7 Impact mapping extract illustrating the weighting of selected critical steps and CMfA

Based on this mapping, the decision was made to focus on the following topics to strengthen the allogeneic process platform:

Formulation, Fill and Finish steps
Cell expansion and purification steps
Processability and manufacturing strategy
Raw material strategy

These select topics of industrialization initiative will be further developed in future publications.

Conclusion & Analysis

Capitalizing on the well-established QbD methodology, Catalent’s Cell Therapy team has developed a complementary methodology – MbD- to address challenges linked to the industrialization of cell-based manufacturing processes.

This methodology was applied to a generic allogeneic T-cell-based process enabling us to rationally select the most critical aspects of industrialization in order to propose a robust, scalable, cost-effective and sustainable allogeneic platform.

One of the key learnings from this exercise was the criticality of the fill and finish operations for allogeneic products. Catalent offers a significant number of allogeneic projects with the intent to offer our customers a state-of-the-art filling platform, that accounts for the specificity of allogeneic products.

In order to strengthen and speed-up the development of this commercial allogeneic process platform, Catalent is looking to establish collaborations with external service providers to develop and integrate advanced technology that will provide solutions for today’s cell therapy manufacturing challenges.

In conclusion, the same MbD methodology described in this study can be adapted to autologous manufacturing processes and analytical testing systems to provide an assessment platform for next-generation manufacturing.

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