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2022 IBIG Forum

Posted by Evotec on Jun 14, 2022 1:31:12 PM

Date: 19-21 October 2022

Location: Evotec Campus Levi-Montalcini, Verona, Italy

 

Evotec will host the 2022 IBIG Forum and the two pre-forum courses at its site in Verona, Italy. 

We are really happy to host this Forum in Verona after two years that the event was held remotely due to the Covid pandemic!

The Forum is organized by the Italian Biostatistics Group(IBIG), a working group of SIMeF (Società Italiana di Medicina Farmaceutica) and is the most important Italian annual meeting congress for biostatisticians, data managers and statistical programmers from the world of industry, independent research and academia.

The two parallel pre-forum (19th October) courses will be:

  • Validation in Statistical Programming: Way of Working QC and Applied Exercises
  • From a Successful Prior Elicitation Meeting to a Reliable Probability of Success Estimate: Quantitative Decision-Making Principles & Practicalities

The Forum (20th -21st October) will be divided into two main sessions:

  • Statistics Beyond Clinical Trials:
    • Artificial Intelligence and Machine Learning for Clinical Research
    • Data Quality and Risk-Based Monitoring
  • Statistics in Clinical Trials:
    • Interim Analysis
    • Estimands & Estimation

Evotec will contribute to the scientific program and acting as moderator as part of the group’s board with our Research Expert Clinical Biostatistician Andrea Nizzardo.

You can register to the Forum here

Registrations to the pre-forum courses can be made here

 

Looking forward to meeting you in Verona on 19-21 October!

 

Download the final programme here

Tags: Events, Evotec

24th International Reid Bioanalytical Forum

Posted by Evotec on Jun 13, 2022 10:26:06 AM

Date: 13-16 June 2022

Location: Cambridge, United Kingdom

Attending: Rossella Cardin (Evotec), Simon Wood (Cyprotex), Ben Smith (Cyprotex) & Basile Khara (Cyprotex)

 

Our scientific program

Poster presentation

“Use of quantitative LC-MS/MS methods to compare conventional blood collection and microsampling in non-human primate” by Rossella Cardin, Evotec

 

Oral presentation

“LC-MS analysis of challenging peptides to support discovery PK” by Basile Khara, Cyprotex

 

If you wish to meet with us at the Reid Bioanalytical Forum, get in touch via the form below, we will be happy to arrange a meeting.



Learn more about the Reid Bioanalytical Forum.

Tags: Events, Cyprotex

AI/ML-Driven Antibody Discovery

Posted by Evotec on Jun 10, 2022 12:18:43 PM

Antibodies generated in the lab are important as potential treatments for a broad spectrum of diseases, in particular infectious diseases caused by viruses. They can be obtained either by animal-derived B cells or from antibody library display platforms. Evotec’s strategy for the optimal path to obtain lead candidates is offering access to both sources of antibodies for discovery, coupled with the exploitation of state-of- the-art technologies to ensure success for a broad range of targets and disease states. In addition, selected lead candidates can be further optimized using powerful computational platforms to enhance productivity, manufacturability, and formulation stability. This is the end-to-end J.Design biologics platform, which is fueled by the front-end discovery platform, J.HAL™ (Just Humanoid Antibody Library) and associated data-driven, company-wide machine learning methodology.

By using artificial intelligence (AI) and machine learning (ML), J.HAL can generate novel, humanoid antibody sequences that both represent natural repertoires and are biased towards desirable features. To enable properties such as broad target and epitope engagement, focused efficacy, and suitable developability, Just-Evotec Biologics has devised an Antibody-GAN (Generative Adversarial Network), a new synthetic approach to designing a novel class of antibody therapeutics, which is termed humanoid antibodies.

At the conferences International Conference on Antiviral Research (ICAR) 2021 and Antibody Engineering & Therapeutics Europe 2022, researchers from Evotec and Just-Evotec Biologics introduced results obtained by using GAN to generate novel sequences, which mimic natural human response and provide the necessary diversity and developability features.


Competing Neural Networks


GAN is based on competing, deep layer neural networks that learn and produce the features of the mature human antibody repertoire, including sequence characteristics and structure properties, allowing for the encoding of key properties of interest into diverse libraries for a feature-biased discovery platform. It works to:

  • capture the complexity of the entire variable region of the standard human antibody sequence space,
  • provide a basis for generating novel antibodies that span a larger sequence diversity than standard in silico generative approaches, and
  • incorporate transfer learning, a critical feature for antibody discovery to bias the physical properties of the generated antibodies towards broader efficacy traits such as CDR lengths and surface properties, improved developability (e.g., improved thermal and pH stability), and diverse chemical and biophysical properties.

The GAN network is trained by using hundreds of thousands of human antibody sequences to recognize legitimate human v-genes. The generator network generates random sequences to fool the discriminator while continually receiving feedback from the discriminator on sequence validity. Over time, the two networks get progressively better at their tasks. After full training, the Antibody-GAN generator is eventually able to produce fully human, novel antibody sequences for the germline for which the GAN was trained.

Antibodies targeting SARS-CoV-2

To demonstrate the usefulness of this platform, the researchers used their newly constructed, 1 billion theoretical diversity phage Fab library with the intent to discover antibodies to the SARS-CoV-2 spike protein. Candidates that specifically bound SARS-CoV-2 spike protein and did not bind an irrelevant antigen were further characterized for dose-dependent binding using AlphaLISA technology. In the primary “yes/no” binding screen a total of 73 unique antibody sequences specific for SARS-CoV-2 spike protein were identified. The researchers then performed binding assays using unpurified transfection supernatants and later reproduced the results with purified material. The candidate antibody supernatants that specifically bound SARS-CoV-2 spike protein were subsequently tested for their ability to block binding of this protein to human ACE-2 receptor. The team identified multiple antibodies that effectively blocked spike human ACE2 receptor interaction, demonstrating the feasibility to screen unpurified transfection supernatants for functional activity. After further rounds of panning, the top candidates expressed at flask scale were purified and tested for SARS-CoV-2 neutralization ability across multiple strains. The researchers identified multiple candidates with neutralizing activity against several strains of SARS-CoV-2. Nine of these antibodies exhibited blocking activity of the spike protein to the ACE2 receptor in an in vitro functional assay. Of note, all antibody data shown here were from native library candidates without any affinity maturation.

The presentation demonstrates that applying machine learning algorithms in antibody discovery “promotes efficient learning from the least expensive and most abundant data encoded in the DNA of antibodies, to validation of this learning through less abundant, more expensive, but most relevant data from GMP manufacturing at full commercial scale,” stated James N. Thomas, retired Executive Vice President, Global Head of Biotherapeutics and President U.S. Operations at Just - Evotec Biologics. “This is a systems approach to platform definition and continuous improvement, and it is unique in the industry, made possible by a number of factors that will be difficult for others to replicate."

To learn more about Evotec's capabilities read our related poster.

Learn More

Tags: Blog, Biologics

AI-derived Antibodies Against SARS-CoV-2 Strains

Posted by Evotec on Jun 10, 2022 11:46:09 AM

Key Takeaways:

  • We have developed an AI-generated antibody library platform, which we call J.HAL®,  utilizing a Generative Adversarial Network (GAN) that generates novel sequences which mimic natural human response, as well biasing toward diversity and developability features.
  • The resulting Humanoid Antibody Library was successfully screened to obtain a panel of novel, diverse and pharmacologically active human antibodies against SARS-CoV-2.

 

DOWNLOAD

Tags: Posters, Biologics

Improving Virus Clearing Studies in Recombinant Protein Production

Posted by Evotec on Jun 10, 2022 11:41:10 AM

Key Takeaways:

  • Non-infectious, purified RVLPs can be used in place of model viruses to predict process performance for viral clearance.
  • Initial screenings show that clearance also trends similarly between bench screenings and higher throughput plate screenings.
  • Plate-based screening of RVLPs in-process can examine up to 24 different run conditions simultaneously and uses less viral surrogate compared to bench scale runs, allowing for greater evaluation and confidence going into formal viral clearance studies.

Improving virus clearing studies in recombinant protein production

Chinese hamster ovary (CHO) cells are the most frequently used mammalian host cells for the industrial manufacturing of recombinant protein therapeutics. They can produce recombinant proteins on the scale of up to 10 gram per liter of culture. However, they are also known to contain type‐C endogenous retrovirus (ERV) sequences in their genome and to release retroviral‐like particles. Although evidence for their infectivity is missing, this has raised safety concerns, and regulatory agencies require demonstration that the purification process removes or inactivates viruses.

Viral clearance validation is assessed through “spiking studies”, whereby model mammalian viruses are introduced into process material which then undergoes the purification technique to be tested. Viral quantity before and after processing is determined through infectivity or qPCR assay. As these studies use live viruses, they require specialized Biological Safety Level laboratories (BSL) and experienced personnel and can create a substantial bottleneck because typically only 3rd party facilities are qualified to perform these studies.

As an alternative, Just - Evotec Biologics is in the early stages of establishing a high-throughput process using commercially available purified retrovirus-like particles from Cygnus Technologies LLC. These particles are non-infectious and mimic the physicochemical properties of live infectious viruses. By using these particles as spiking agents, the retroviral clearance capability of downstream unit operations can be studied, assessed, and quantified by reverse transcriptase quantitative polymerase chain reaction (RT-qPCR). Usually, this is performed at bench scale using chromatography columns.

In a poster presented at this year’s ACS spring conference entitled High throughput optimization of chromatography steps for viral clearance using retrovirus-like particles (RVLPs), researchers from Just-Evotec Biologics detailed the high-throughput workflow for the analysis of RVLP content for rapid analysis of in-process samples.

The research team compared common bench scale chromatography runs with a plate-based screen using resin-loaded filter plates and a liquid handling robot. While at bench scale, only a single set of run conditions can be tested at a time, the plate-based screening can examine up to 24 different run conditions simultaneously. It also uses less RVLP stock solution. The researchers expect that plate-based screening of RVLPs will not only save time and costs, but also allows for better evaluation and confidence before formal viral clearance studies.

 

DOWNLOAD

Tags: Posters, Biologics

34th EORTC-NCI-AACR Symposium

Posted by Evotec on Jun 8, 2022 8:47:07 AM

Date: 26-28 October 2022

Location: CCIB, Barcelona, Spain

Attending: Sandrine Delbary, Anne-Sophie Casagrande, Fred Somny

 

If you wish to meet with us in Barcelona, get in touch via the form below, we will be happy to arrange a meeting.


Learn more about the 34th EORTC-NCI-AACR Symposium.

Tags: Events, Evotec

iPSC and Age-Related Diseases: Case Study Age-Related Macular Degeneration

Posted by Evotec on May 31, 2022 11:53:48 AM

iPSC and age-related diseases: Case study AMD
Age-related macular degeneration (AMD) is a leading cause of vision loss in people over the age of 50, accounting for 90% of blindness in this population. There are dry and wet forms of the disease and to date, there are limited treatment options for the wet form and none for dry AMD. The exact cause of the disease is unknown, but it is suspected that it results from a combination of hereditary and environmental factors, with smoking and diet being implicated. Globally, more than 190 million people are affected by AMD and this figure is expected to increase to more than 285 million by the year 2040. The estimated global cost of the disease currently stands at $343bn, with $255bn in direct healthcare costs.

Significant research effort has been targeted towards identification of the genes involved in permanent vision loss through photoreceptor and/or retinal pigment epithelium (RPE) cell dysfunction or cell death. So far, mutations in over 250 genes are known to be involved. Despite a good understanding of the genotype-phenotype relationship in AMD, this has not translated into predictive in vitro and in vivo models to understand disease mechanisms.

Partnership on iPSC-derived RPE cells
To drive the search for treatments for this devastating disease, it is vital to identify and develop new models which enable elucidation of retinal disease mechanisms and reliably predict the efficacy of therapeutic compounds. To address these challenges, Evotec has teamed up with the Centre for Regenerative Therapies (CRTD) in Dresden, Germany. The CRTD has a longstanding interest in degenerative processes and has contributed significantly to our understanding of retinal diseases in recent years. The joint TargetRD project is based on Evotec’s know-how in induced pluripotent stem cell (iPSC) technology, generating iPSC-derived RPE cells from AMD patients.

RPE cells are essential for visual function and a key component for light detection by photoreceptor neurons. They also are crucial for maintaining the blood-retina-barrier, for the transport of diverse biomolecules, ions, and fluids in and out of the retinal tissue, and recycling of the visual chromophore retinal molecule.

Even more important is their ability for phagocytosis: A single RPE cell is in contact with about 30 photoreceptor cells and responsible for the phagocytosis and removal of the distal portions of the photoreceptor outer segments that are phagocytozed in the course of a day. This is an important process with up to 10% eliminated daily, meaning the entire population of photoreceptor outer segments is turned over every 2 weeks. Maintaining, repairing, or replacing RPE cells therefore is crucial for the management of AMD, but also for other retinal degenerative diseases.

So far, research has been hampered by limited access to RPE cells. There are immortalized retinal cell lines available, but they lack the typical cell morphology or function of their in vivo counterparts, e.g. pigmentation, polarization, and expression of certain proteins. Likewise, artificial organoids, so-called 3D-cups, are not ideal since they are difficult to grow and differentiate and not suited for high-throughput profiling of compounds.

This situation is now improving as Evotec and CRTD succeeded in developing a protocol to efficiently and robustly produce high quality human iPSC-derived RPE cells at industrial scale from patient cells. This means that partners can not only investigate disease pathology directly in this highly relevant retinal cell type but for the first time also study disease phenotypes and mechanisms within the context of a patient’s genome. Moreover, the TargetRD platform enables the study of individual, overlapping functional and morphological changes from iPSC-RPE cells derived from patients with different genetic backgrounds, providing an opportunity to unravel complex AMD disease phenotypes.

Promising first results
Already, the partners were able to show the utility of the TargetRD platform by analyzing iPSC-RPE cells carrying a patient mutation resulting a lysosomal storage disorder. Amongst other symptoms, patients with this type of mutation develop severe retinal degeneration, leading to complete blindness early in life. Using the various phenotypic and functional assays established, it was possible to demonstrate impaired trans-epithelial resistance in patient cells. This indicates that in this case, patient RPE cells are unable to form the tight monolayer required for normal RPE cell function. Furthermore, patient RPE cells have, as expected, impaired lysosomal activity and are unable to phagocytose photo- receptor outer segments (POS) at the same rate as control RPE cells. Since all assays are able to support high-throughput screening, the partners can use the TargetRD platform to identify phenotypic and functional disease phenotypes from patient cells, enabling novel drug discovery approaches.

Furthermore, the project combines Evotec’s drug discovery expertise and the academic excellence of the CRTD to achieve significant progress towards developing therapies much needed by the patients.

Both partners believe this is a very promising approach that enables successful drug discovery programs for retinal degenerations coupled to a high likelihood of successful translation into the clinic.

Tags: Blog, Biologics, Age-Related Diseases

Inspiring insights in Biotechnology – today, tomorrow, together

Posted by Evotec on May 31, 2022 10:57:18 AM

Date: 08th June, 2022

Location: Alderley Park, Macclesfield, Cheshire SK10 4TG

Attendee: Benjamin Park

Presentation: Building Comprehensive in vitro Methods to Evaluate Pre Clinical Drug Toxicity

Learn more about Inspiring insights in Biotechnology – today, tomorrow, together

Tags: Events, Cyprotex

EMBO Workshop - Tuberculosis 2022

Posted by Evotec on May 30, 2022 9:45:37 AM

Date: 12-16 September, 2022

Location: CIS auditorium, Institut Pasteur, Paris, France

Attending: Anna Upton SVP R&D Tuberculosis, Global Infectious Diseases

 

Join Evotec at EMBO Workshop about Tuberculosis!

 

If you wish to meet with us in Paris, get in touch via the form below, we will be happy to arrange a meeting.

Learn more about the EMBO Workshop.

Tags: Events, Evotec

Antiviral Capabilities at Evotec

Posted by Evotec on May 26, 2022 8:18:40 PM

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Tags: SP Standalone