On October 31, 2023 SOTIO Biotech, a clinical-stage immuno-oncology company owned by PPF Group, reported that it will be presenting new preclinical data at the Society for Immunotherapy of Cancer (SITC) (Free SITC Whitepaper)’s 38th Annual Meeting taking place November 1-5, 2023 in San Diego, California (Press release, SOTIO, OCT 31, 2023, View Source [SID1234636599]).

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Data to be presented include new preclinical results supporting the continued development of SOT201, a next-generation PD-1-inhibiting cytokine that SOTIO is progressing toward a planned first-in-human study in the second quarter of 2024. SOT201 is an antibody-cytokine fusion protein that could improve upon the efficacy of approved checkpoint inhibitors by combining PD-1 blockade with IL-15 immune stimulation in a single therapeutic construct.

Additional poster presentations at the meeting will include preclinical data on the synergistic effects of SOTIO’s IL-15 superagonist in combination with CAR T-cell therapies, as well as data on SOTIO’s IL-15 superagonist nanrilkefusp alfa.

Presentation details are as follows:

Title: "SOT201 is a novel cis-acting immunocytokine targeting IL-15Rβγ and PD-1 to reinvigorate PD-1+ tumor infiltrating lymphocytes and potentiate anti-tumor efficacy"
Number: 1087
Date: November 3, 2023
Presenter: Irena Adkins, Martin Steegmaier

Title: "Combination with IL-15Rβγ superagonist, Nanrilkefusp alfa, enhances CAR T and BOXR T cell anti-tumor activity"
Number: 815
Date: November 3, 2023
Presenter: Amy Jensen-Smith

Title: "Nanrilkefusp alfa, a high-affinity IL-15Rβγ agonist, promotes an innate and adaptive anti-tumor inflammatory environment as single agent or combined with anti-PD-1 in patients with advanced cancers"
Number: 713
Date: November 3, 2023
Presenter: Petr Danek, Lenka Palova Jelinkova

Posters will be available after presentations conclude HERE.

On October 31, 2023 Capstan Therapeutics, Inc. ("Capstan"), a biotechnology company dedicated to advancing in vivo reprogramming of cells through RNA delivery utilizing targeted lipid nanoparticles (tLNP), reported that it will present preclinical data showing rapid and robust anti-tumor and anti-primary B cell activity in humanized mice by tLNP administration delivering an mRNA encoding an anti-CD19 chimeric antigen receptor (CAR), at the Society for Immunotherapy of Cancer (SITC) (Free SITC Whitepaper) 38th Annual Meeting in San Diego, California (Press release, Capstan Therapeutics, OCT 31, 2023, View Source [SID1234636598]).

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"These data highlight the potential for Capstan’s targeted LNP-mRNA platform to provide a truly disruptive, off-the-shelf, cell-free, scalable and tunable solution for patients without the need for harsh lymphodepletion conditioning or viral vectors that are required for conventional ex vivo cell therapies," said Adrian Bot, M.D., Ph.D., Capstan’s Chief Scientific Officer, and Executive Vice President of R&D. "We have demonstrated efficient and therapeutically relevant delivery of mRNA CAR payloads to human T cells. This resulted in rapid and profound pharmacodynamic effect in two mouse models, comprising eradication of human primary B cells or Nalm6 leukemic cells, respectively. These data provide a springboard for developing novel, in vivo CAR therapies that may overcome access and clinical performance issues with currently available ex vivo CAR therapies, with broad applicability in autoimmune and oncology indications."

Poster Details:

Title: In vivo engineering of CAR T cells using a novel targeted LNP-mRNA technology
Presentation type: Poster
Session: Poster Hall
Date and time: Saturday, November 4, 2023: 9:00 AM – 8:30 PM
Lead authors: Gregor Adams, Ph.D., and Haig Aghajanian, Ph.D.

A copy of the poster will be added to the "Publications and News" section of Capstan’s website at www.capstantx.com/.

On October 31, 2023 Affini-T Therapeutics, Inc., a precision immunotherapy company unlocking the power of T cells against oncogenic driver mutations, reported that preclinical data from its oncogenic driver program targeting KRAS G12D, AFNT-212, will be presented at the Society for Immunotherapy of Cancer (SITC) (Free SITC Whitepaper) 38th Annual Meeting (Press release, Affini-T Therapeutics, OCT 31, 2023, View Source [SID1234636597]).

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"Gene editing is a key piece of our overall strategy to develop precision immunotherapies for patients with hard-to-treat solid tumors," said Loïc Vincent, Ph.D., Chief Scientific Officer, Affini-T Therapeutics. "Our data show that non-viral targeted knock-in engineered AFNT-212 T cells drive a robust coordinated CD4+ CD8+ T cell immune response against KRAS G12D mutated tumors with promising preclinical activity and tolerability, supporting the planned clinical development of our AFNT-212 T Cell Receptor-engineered therapy. We look forward to presenting these findings at SITC (Free SITC Whitepaper)."

Poster presentation details are as follows:

Title: Directing a high avidity KRAS G12D-specific TCR engineered with a CD8αβ co-receptor and chimeric cytokine receptor using non-viral knock-in enhances anti-tumor responses
Abstract no: 355
Presenting Author: Ankit Gupta, Ph.D., Senior Director, Gene Editing, Affini-T Therapeutics
Date/Time: Friday, November 3, 2023, 12:00 pm – 1:30 pm and 5:10 pm – 6:40 pm PT

Title: Non-viral targeted knock-in of a KRAS G12D specific TCR, CD8αβ, and chimeric cytokine receptor in the TRAC locus outperforms lentiviral-based engineering of T cells
Abstract no: 1223
Presenting Author: Allison P. Drain, Ph.D., Senior Scientist, Synthetic Biology, Affini-T Therapeutics
Date/Time: Friday, November 3, 2023, 12:00 pm – 1:30 pm and 5:10 pm – 6:40 pm PT

On October 31, 2023 -Incendia Therapeutics, a precision oncology company discovering and developing a novel class of therapies that reprogram the tumor microenvironment (TME), reported that it will present three posters at the Society for Immunotherapy of Cancer (SITC) (Free SITC Whitepaper) 38th Annual Meeting, to be held in San Diego, California November 1-5, 2023 (Press release, Incendia Therapeutics, OCT 31, 2023, View Source [SID1234636596]).

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Early/Late Stage Pipeline Development - Target Scouting - Clinical Biomarkers - Indication Selection & Expansion - BD&L Contacts - Conference Reports - Combinatorial Drug Settings - Companion Diagnostics - Drug Repositioning - First-in-class Analysis - Competitive Analysis - Deals & Licensing

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"We look forward to presenting three posters at SITC (Free SITC Whitepaper) which validate our approach to block Discoidin Domain Receptor 1 (DDR1) and advance our understanding of and ability to detect immune exclusion in solid tumors," said Laura Dillon, PhD, VP, Translational Medicine & Bioinformatics at Incendia Therapeutics. "We are encouraged by the human tumor data in intrahepatic cholangiocarcinoma (iCCA), which demonstrate a correlation of high DDR1 expression with worse prognosis in all stages of disease. The prevalence of high DDR1 expression and poor survival outcomes associated with this make iCCA a relevant tumor type for evaluating novel DDR1-targeted therapies."

Presentation Details for SITC (Free SITC Whitepaper) 2023 are as follows:

Title: DDR1 expression is associated with a worse prognosis in intrahepatic cholangiocarcinoma
Poster number: 1486
Presenter: Travis Clifton, MD, Co-founder, Head of Clinical Sciences
Time: Saturday, November 4, 12:15-1:45 PM PDT and 5:30-7:00 PM PDT (3:15-4:45 PM EDT and 8:30-10 PM EDT)
Location: Poster Hall (Exhibit Hall B)

Title: The epithelium-stroma interface serves as a barrier to immune cell infiltration across tumor immune phenotypes in epithelial cancers
Poster number: 1497
Presenter: Laura Dillon, Ph.D., VP, Translation Medicine & Bioinformatics
Time: Friday, November 3, 12:15-1:45 PM PDT and 5:30-7:00 PM PDT (3:15-4:45 PM EDT and 8:30-10 PM EDT)
Location: Poster Hall (Exhibit Hall B)

Title: Comparison of multiplex immunofluorescence and H&E-based approaches for characterization of the tumor microenvironment
Poster number: 1287
Presenter: Fredrick Gootkind, M.S., Senior Associate Scientist
Time: Friday, November 3, 12:15-1:45 PM PDT and 5:30-7:00 PM PDT (3:15-4:45 PM EDT and 8:30-10 PM EDT)
Location: Poster Hall (Exhibit Hall B)

On October 31, 2023 Asher Biotherapeutics, a biotechnology company developing precisely-targeted immunotherapies for cancer, autoimmune, and infectious diseases, reported new preclinical data for AB821, its CD8-targeted interleukin-21 (IL-21) immunotherapy (Press release, Asher Biotherapeutics, OCT 31, 2023, View Source [SID1234636595]). The data will be presented at the Society for Immunotherapy in Cancer (SITC) (Free SITC Whitepaper) 38th Annual Meeting, being held in San Diego, CA on November 1-5, 2023.

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"We are pleased to share new preclinical data for AB821 at SITC (Free SITC Whitepaper), further illustrating the potential of our highly differentiated cis-targeted immunotherapies for the treatment of cancer," said Andy Yeung, Ph.D., Chief Technology Officer and Co-founder of Asher Bio. "IL-21 has historically demonstrated promising antitumor activity, but its clinical use has been limited due to toxicities and pleiotropic effects. We designed AB821 to activate only CD8+ T cells, the immune cell type driving the antitumor response, potentially maximizing the efficacy of IL-21 and limiting off-target activity. The new preclinical data presented at SITC (Free SITC Whitepaper) demonstrate that AB821 can improve the functionality of exhausted CD8+ T cells and promote their function and survival to effectively facilitate potent antitumor activity. Based on these data, we believe AB821 could significantly improve the treatment paradigm for patients with tumor types unresponsive to checkpoint blockade therapies, who typically have highly exhausted CD8+ T cells in their tumors. We look forward to advancing AB821’s clinical development and remain on track to file an IND in the fourth quarter of 2023."

New Preclinical Data for AB821, Asher Bio’s CD8-Targeted IL-21

In a poster presentation entitled, "AB821 is a CD8+ T cell selective IL-21 with enhanced bioavailability that reduces CD8+ T cell exhaustion to induce potent antitumor activity," lead author Renee Greer, Ph.D., Principal Scientist at Asher Bio, described new preclinical data further characterizing the mechanisms by which AB821 enhances the functionality of CD8+ T cells and facilitates the antitumor effects of IL-21, further supporting AB821’s development. The data show:

A murine surrogate of AB821 (muAB821) demonstrated potent antitumor activity both as a monotherapy and in combination with anti-PD-1 therapy in anti-PD-1 refractory mouse tumor models.
Exhausted CD8+ T cells are a promising target for AB821 therapy, as supported by the following:
High levels of IL-21R were observed in the exhausted CD8+ T cell subset in mouse tumors and in human tumor-infiltrating lymphocytes (TILs)
Treatment with muAB821 resulted in replacement of exhausted CD8+ T cells with CD8+ T cells with restored cytotoxic potential and expressing memory markers.
In human TILs, exhausted CD8+ T cells were shown to be highly responsive to treatment with AB821 as measured by pSTAT3 sensitivity.
In human TILs cultured with AB821, AB821 acted on exhausted CD8+ T cells to improve their antitumor functionality by increasing expression and secretion of key effector proteins such as Granzyme B and perforin, both of which are essential for antitumor activity.
Clinical Trial in Progress for AB248, Asher Bio’s CD8-Targeted IL-2

Also at SITC (Free SITC Whitepaper), a poster highlighting Asher Bio’s lead immunotherapy candidate, AB248, a CD8+ T cell-selective IL-2, will be featured in a clinical trial in progress poster. The poster, entitled "An open-label, Phase 1a/b study of AB248, a CD8+ T selective IL-2 mutein fusion protein, alone or in combination with pembrolizumab in patients with advanced solid tumors," details the design of the ongoing Phase 1a/1b study of AB248 alone and in combination with pembrolizumab in patients with advanced solid tumors who failed prior standard of care treatments (NCT05653882). Asher Bio initiated this Phase 1a/1b study in January 2023.

Both poster presentations will be available in the "Presentations and Posters" section of Asher Bio’s website: View Source

About AB821

IL-21 is a cytokine that activates STAT3, a master transcription factor involved in a broad spectrum of adaptive and innate immune functions. In oncology, IL-21 has historically demonstrated promising in early clinical studies, but was hindered by toxicities and pleiotropic effects, such as suppression of antigen presentation, which could dampen overall antitumor efficacy. Asher Bio hypothesized that focusing the activity of IL-21 to only the immune cell type primarily responsible for antitumor efficacy, while avoiding activation of other cells, would maximize the efficacy potential of IL-21 and reduce toxicity. Like IL-2, IL-21 derives its benefit from stimulating CD8+ T cells, but it mediates antitumor activity via a distinct, potentially complementary pathway. Asher Bio developed AB821 as a cis-targeted IL-21 activating cytokine that selectively targets CD8+ T cells, the immune cell type driving antitumor response. The IL-21 activating cytokine promotes cytotoxicity, memory cell differentiation, survival and reinvigoration of CD8+ T cells, all of which support antitumor activity. Asher Bio believes that AB821 has the potential to treat tumor types that may not be responsive to IL-2 and/or PD-1 therapy. PD-1-resistant tumors are associated with reduced memory T cell numbers and increased exhausted T cell numbers, suggesting that this molecule may be beneficial in these resistant tumors. AB821 also has the potential to be used in combination with AB248 to enhance efficacy by combining a proliferation signal with one that optimizes functionality and prevents T cell exhaustion.