On April 7, 2023 A regulatory class of human T cells descended from two different origins, one that relates to autoimmunity and one that relates to protective immunity, reported by a new study led by Children’s Hospital of Philadelphia (CHOP) (Press release, CHOP, APR 7, 2023, View Source [SID1234629890]). The findings, published today in Science Immunology, could pave the way for new treatments for autoimmune diseases that target the immune system selectively.

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"When it comes to autoimmunity, the prevailing wisdom has been that the only way to stop inflammation is to suppress the immune system broadly, making patients more susceptible to infection," said senior author Neil D. Romberg, MD, an attending physician in the Division of Allergy and Immunology at Children’s Hospital of Philadelphia. "However, that is only true if all T cells come from the same place. What this study shows is that there are two different T cell lineages, which means you might be able to have your cake and eat it too – suppressing inflammation due to autoimmunity while allowing T cells that fight infection to thrive."

Germinal centers (GCs) are spherical collections of cells inside tonsils, lymph nodes, and the spleen that orchestrate interactions between T follicular helper (Tfh) cells and B cells. The action within these GCs is locally governed by FOXP3+ T follicular regulatory (Tfr) cells. Although the proper function of Tfr cells is likely important to immunologic health – and their dysfunction a potential contributor to various disease states – few studies have assessed the biologic roles of human Tfr cells and none have addressed where they come from or how they develop within tissues.

To solve this problem, the researchers, led by Carole Le Coz, PhD, a former postdoctoral researcher in the Romberg Lab, used a combination of computational, in vitro, and in vivo techniques to describe the origins, functions, and positions of Tfr cells within GCs. Since GCs are located in secondary lymphoid tissues like lymph nodes, spleens, and tonsils, the researchers analyzed tonsils that had been removed from healthy donor patients.

Using an interlocking suite of single cell technologies, the researchers were able to show that there is one subpopulation of Tfr cells that is induced by Tfh cells, which they called iTfrs, and another subpopulation that were "naturally" derived from Tregs, a subpopulation of T cells that are responsible for moderating the immune system, which they called nTfrs. In doing so, the demonstrated that there are two developmental trajectories: Treg-to-nTfr and Tfh-to-iTfr.

Once the researchers identified these two subpopulations of Tfr cells, they analyzed whether these two regulatory T cells express the surface protein CD38 differently. They found that iTfr cells express CD38, whereas nTfr cells do not. They were also able to catalogue the precise location of these different subpopulations within the GCs, in addition to demonstrating their developmental path and ability so support B cell function.

"This study raises the question of whether we could selectively deplete iTfr cells through anti-CD38 treatments, while leaving nTfrs intact – using a silver bullet rather than a bomb to target specific T cells," Dr. Romberg said. "A similar approach could also potentially be used in a therapeutic context to boost immunity in patients with weakened immune systems."

This work was supported by grants from the National Institutes of Health, National Institute of Allergy and Infectious Diseases (AI146026), National Institute of Allergy and Infectious Diseases (AI155577, AI115712, AI117950, AI108545, CA210944, AI114852), National Heart, Lung, and Blood Institute (R38 HL143613, T32 HL 7775-28), and the National Cancer Institute (T32 CA009140). Additional funding was provided by the Parker Institute for Cancer Immunotherapy, the Parker Bridge Fellow Award, the Gray Foundation, the Chan Zuckerberg Initiative Pediatric Networks for the Human Cell Atlas, the Gail B. Slap Department of Pediatrics Fellowship Award, and the Sayer family.

Le Coz et al. "Human T follicular helper clones seed the germinal center-resident regulatory pool," Science Immunology, April 7, 2023, DOI: 10.1126/sciimmunol.ade8162

On April 7, 2023 Molecular Templates, Inc. (Nasdaq: MTEM, "Molecular Templates," or "MTEM"), reported that the U.S. Food and Drug Administration (the "FDA") informed MTEM that it has placed a partial clinical hold on the Phase 1 study of MT-0169 based on previously disclosed cardiac adverse events noted in two patients dosed at 50 mcg/kg that prompted the dose reduction to 5 mcg/kg last year (Press release, Molecular Templates, APR 7, 2023, View Source [SID1234629887]). Since then, four patients have been dosed at 5 mcg/kg and three patients have been dosed at 10 mcg/kg with no cardiac adverse events noted.

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Of the patients dosed at 50 mcg/kg, one patient experienced asymptomatic grade 2 myocarditis and one patient experienced asymptomatic grade 3 cardiomyopathy; both patients had full recoveries within two months of these events. No grade 4 or 5 toxicities were observed at 50 mcg/kg. Under the partial clinical hold, current study participants may continue treatment, but no new patients will be enrolled until the partial hold is lifted by the FDA.

After filing a protocol amendment in January 2022, Molecular Templates resumed study treatment in patients with relapsed Multiple Myeloma at 5 mcg/kg, a 90% reduction in dose. Four patients were dosed at 5 mcg/kg with no adverse events greater than grade 1 noted and no cardiac adverse events noted. One patient dosed at 5 mcg/kg had a Very Good Partial Response ("VGPR") that deepened to a stringent complete response and remains on study for more than 7 months. Three patients were dosed at 10 mcg/kg with no cardiac events noted; one patient dosed at 10 mcg/kg experienced transient grade 2 diarrhea.

The FDA has asked MTEM to provide narratives on the two patients who experienced cardiotoxicity at 50 mcg/kg, justification for the revised dose of 5 mcg/kg, and data evaluating the clinical benefit-to-risk ratio seen with the lower doses of MT-0169, among other requests.

"Patient safety is our highest priority. The 5 and 10 mcg/kg cohorts have been completed and we have not observed any cardiac adverse events or other serious adverse events at these lower doses. One patient dosed at 5 mcg/kg is in a stringent complete response and is in his seventh month of therapy. We look forward to sharing these data with the FDA and are confident in the benefit-risk profile of MT-0169 at these lower doses," said Roger Waltzman, MD., Chief Medical Officer at MTEM. "We are excited to see early signs of clinical benefit in this difficult-to-treat patient population."

On April 7, 2023 Seagen Inc. (Nasdaq: SGEN) reported that it will report its first quarter 2023 financial results on Thursday, April 27, 2023 (Press release, Seagen, APR 7, 2023, View Source [SID1234629885]).

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Given the recently announced agreement to be acquired by Pfizer Inc., Seagen will not be hosting a conference call.

On April 7, 2023 M2GEN, an oncology-focused health informatics solutions company, reported its participation as a presenter, exhibitor, and research partner at the American Association for Cancer Research (AACR) (Free AACR Whitepaper) Annual Meeting April 14-19, in Orlando, Florida (Press release, M2Gen, APR 7, 2023, View Source [SID1234629883]). Eight poster presentations and one oral presentation will be presented at AACR (Free AACR Whitepaper), utilizing the lifetime patient-consented longitudinal clinicogenomic data from M2GEN’s Oncology Research Information Exchange Network (ORIEN) Avatar program, showcasing the collaboration of scientists across ORIEN, M2GEN, and other leading cancer centers across the nation.

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These projects highlight research discoveries in pancreatic, bladder and multiple myeloma, and defining biomarkers that predict the therapeutic benefits with immune checkpoint inhibitors. Partnering with our 18 ORIEN members, M2GEN enables breakthrough scientific research to advance patient care by utilizing the richest real-world dataset in oncology, comprised of whole exome sequencing (WES), whole transcriptome sequencing (WTS), germline data, and lifetime clinical patient data.

"Spanning 18 of the nation’s top cancer centers, our network’s cornerstone is collaborative research and we’re excited to have several of our highly engaged working groups presenting their findings at AACR (Free AACR Whitepaper)23," said Ahmad A. Tarhini, MD, PhD and Chair, ORIEN Scientific Committee & ORIEN Immuno-Oncology RIG and Director, Cutaneous Clinical & Translational Research at H. Lee Moffitt Cancer Center and Research Institute. "We are delighted that work from my group stemming from our ORIEN Immuno-Oncology Research Interest Group will be shared on Tuesday during an oral session focused on studies aimed at identifying better prognostic and predictive biomarkers of benefit from immunotherapies and defining mechanisms of immune resistance. We are hopeful our work will lead to a novel spectrum of tumor-based biomarkers for predicting response and toxicity risks with immune modulator therapeutics."

We look forward to meeting with colleagues, researchers, partners, and future clients individually and at our booth #1301 during the conference. To inquire about partnering with M2GEN and ORIEN, or to learn more about how our rich longitudinal clinicogenomic ORIEN AVATAR dataset could support your research efforts, contact [email protected].
The schedule of ORIEN presentations at AACR (Free AACR Whitepaper) 2023 includes:

Monday, April 17

Bioinformatics Applications in Cancer Biology 1 – Poster Session
Suhn K Rhie, PhD, of University of Southern California will present a poster entitled "The exploratory analysis of dysregulated transcription factor FOXC1 in pan-cancer" (Abstract: 2060 / 29: Full Text).

Bioinformatics Applications in Cancer Biology 2 – Poster Session
Mackenzie D. Postel, MD/PhD candidate at Keck School of Medicine of USC will present a poster entitled "Molecular and clinical correlates of genetic ancestry in a diverse, admixed cancer dataset" (Abstract: 3117 / 3: Full Text).

Tuesday, April 18

Immune-based Biomarkers for Prognostic and Predictive Benefit – Minisymposium
Tingyi Li, MS, will present an oral presentation entitled "The immune cell state atlas analysis predicts therapeutic benefits with immune checkpoint inhibitors" (Abstract: 5703: Full Text).

Drug Resistance in Molecular Targeted Therapies 4 / Regulation of Gene Expression in Drug Resistance – Poster Session
Emmanuelle Hodara, MD/PhD candidate at Keck School of Medicine of USC will present a poster entitled "M6A RNA modifications regulate expression of transcripts that promote transition to cisplatin resistance in bladder cancer" (Abstract: 3908 / 27: Full Text).

Inflammation and Tumor Progression Poster Session
Shankar Suman, PhD of Ohio State University will present a poster entitled "High intratumoral levels of Notch3 increase tumorigenesis and promote an immunosuppressive TME in EGFR-mutant NSCLC" (Abstract: 4650 / 7: Full Text).

Biomarkers of Therapeutic Benefit 5 – Poster Session
Francesco Maura, MD, will present a poster entitled "Individualized risk stratification in newly diagnosed multiple myeloma" (Abstract: 5453 / 3: Full Text).

Wednesday, April 19

Multi-omics Tumor Profiling – Poster Session
Bing-Jian Feng, PhD, will present a poster session entitled "Germline and somatic genomic profiling of urothelial carcinoma" (Abstract: 6074 / 14: Full Text).

Interactions Between the Microbiome, Cancer Cells, and Tumor Stromal – Poster Session
Caroline E. Wheeler will present a poster session entitled "Intra-tumor microbes identified by RNAseq improve predictions of response to immune checkpoint blockade in metastatic melanoma" (Abstract: 5904 / 15: Full Text).

Interactions Between the Microbiome, Cancer Cells, and Tumor Stromal – Poster Session
Daniel Spakowicz, PhD, MS, MPhil, will present a poster session entitled "The tumor microbiome associates with features of the tumor microenvironment, treatment outcomes, and histologies; a national collaboration of the exORIEN Consortium" (Abstract: 5907 / 18: Full Text).

On April 7, 2023 HiFiBiO Therapeutics, a clinical-stage multinational biotherapeutics company, reported that its scientific work in exploring approaches to target the TIGIT/CD226 axis has been selected for oral presentation at the AACR (Free AACR Whitepaper) 2023 meeting during April 14-19, 2023, in Orlando, FL (Press release, HiFiBiO Therapeutics, APR 7, 2023, View Source [SID1234629882]).

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"To date, the industry has struggled to successfully develop therapeutics targeting TIGIT, both as a monotherapy and in combination with anti-PD-1/PD-L1 blockers to effectively stimulate the CD226 axis. We believe the next generation of therapies modulating the CD226 axis will need to target additional immune receptors in the axis," said Jinping Gan, VP Global Head of Research at HiFiBiO Therapeutics. "Through our single cell driven DIS platform, we have made great progress developing multi-specific approaches for CD226 axis immune modulation in addition to understanding the single cell biology in the tumor microenvironment for indication selection and predictive biomarkers."

"Beyond our three immune-oncology clinical programs targeting TNFR2, OX40, and BTLA, we continue to explore how the HiFiBiO DIS approach can transform the drug discovery and development paradigm by integrating deep understanding of immune modulation with a world-leading single cell platform and machine learning-enabled data analysis," said Francisco Adrian, Chief Scientific Officer of HiFiBiO Therapeutics.

Details on the oral presentation are as follows:

Title: Maximizing the outcome of CD226 stimulation through targeting beyond TIGIT signaling with combination and multi-specific approaches for cancer and immunotherapy

Presenter: Jinping Gan, Ph.D., Vice President, Global Head of Research

Session Title: Immune Checkpoints at Tumor Beds

Session Date and Time: Monday, April 17, 2023; 2:30 pm – 4:30 pm

Venue: Valencia D – Convention Center