Immunology and Biotherapies
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Biosimilars -- clinical perspectives in rheumatology - EurekAlert (press release)

Biosimilars -- clinical perspectives in rheumatology - EurekAlert (press release) | Immunology and Biotherapies | Scoop.it
Rheumatologists from Charité -- Universitätsmedizin Berlin and the University of Massachusetts Medical School have been analyzing clinical data on biosimilars that have already been approved for use.
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Immunology and Biotherapies
Page Ressources et Actualités du DIU immunologie et biothérapies
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Resources for DIU Immunologie et Biothérapies

DIU Immunologie et Biotherapies is a french diploma associating french universities and immunology laboratories. It is dedicated to the involvement of immunology in new biotherapies, either molecular or cellular.

Gilbert C FAURE's insight:

We use Scoop.it as preferred curation tool to collect, select, comment informations flowing on the web in this rapidly evolving theme to keep teachers abreast of scientific knowledge and help students surf the wave...                                                            Feel free to be a follower!

 

If you are interested

in Immunology also use http://www.scoop.it/t/immunology

in Mucosal Immunity http://www.scoop.it/t/mucosal-immunity

in Flow Cytometry and Cytomics http://www.scoop.it/t/from-flow-cytometry-to-cytomics

in Allergy an Clinical Immunology http://www.scoop.it/t/allergy-and-clinical-immunology

in Autoimmunity http://www.scoop.it/t/autoimmunity

 

For further information on Immune monitoring of Immune therapies, 

http://www.scoop.it/t/immune-monitoring-1     by MdC

 

Looking for cancer applications inside this topic, use

http://www.scoop.it/t/immunology-and-biotherapies?q=cancer

 

Looking for cytokines and chemokines, use

http://www.scoop.it/t/cytokines-et-chimiokines

 

Thanks to K Maggon for joining us. @Krishan Maggon

 

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Pedro Morais on LinkedIn: #oligonucleotide #steatohepatitis

Pedro Morais on LinkedIn: #oligonucleotide #steatohepatitis | Immunology and Biotherapies | Scoop.it
“#Oligonucleotide Therapies for Nonalcoholic #Steatohepatitis”

Cell Press link: https://lnkd.in/eWwMNyCw
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‘Mini liver’ will grow in person’s own lymph node in bold new trial

‘Mini liver’ will grow in person’s own lymph node in bold new trial | Immunology and Biotherapies | Scoop.it
Biotechnology firm LyGenesis has injected donor cells into a person with liver failure for the first time.
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Frederic CAROFF on LinkedIn: #shingles #tlr4

Frederic CAROFF on LinkedIn: #shingles #tlr4 | Immunology and Biotherapies | Scoop.it
Protection results from GSK Shingrix vaccines against #Shingles are impressive. Guess which adjuvant was used?

👉A #TLR4 agonist of course 🦠

The results…
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Vaccination et Lien Social on LinkedIn: #zona #varicelle #infection #effetsindésirables #prévention #has…

Vaccination et Lien Social on LinkedIn: #zona #varicelle #infection #effetsindésirables #prévention #has… | Immunology and Biotherapies | Scoop.it
🔸 Actualisation de la stratégie vaccinale contre le zona :

Le zona, causé par la réactivation du virus varicelle-zona, est une maladie virale touchant…
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Paulo Rodrigues Santos on LinkedIn: Development of NK cell-based cancer immunotherapies through receptor…

Paulo Rodrigues Santos on LinkedIn: Development of NK cell-based cancer immunotherapies through receptor… | Immunology and Biotherapies | Scoop.it
"The modulation of cytokines and cytokine receptors is highly promising for enhancing NK cell survival and persistence, thus paving the way for durable…
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https://www.cell.com/immunity/abstract/S1074-7613(24)00083-9

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Cédric Gollion on LinkedIn: Bravo à nos collègues de Barcelone qui ont démontré le bénéfice…

Cédric Gollion on LinkedIn: Bravo à nos collègues de Barcelone qui ont démontré le bénéfice… | Immunology and Biotherapies | Scoop.it
Bravo à nos collègues de Barcelone qui ont démontré le bénéfice medico-économique du remboursement des anti-CGRP en Espagne, notamment grâce à la réduction de…
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Tizveni | European Medicines Agency

OverviewOn 22 February 2024, the Committee for Medicinal Products for Human Use (CHMP) adopted a positive opinion, recommending the granting of a marketing authorisation for the medicinal product Tizveni, intended for the treatment of locally advanced or metastatic non-small cell lung cancer (NSCLC) either in monotherapy or in combination with chemotherapy. The applicant for this medicinal product is Beigene Ireland Limited.Tizveni will be available as a 100 mg concentrate for solution for infusion. The active substance of Tizveni is tislelizumab, an antineoplastic agent (ATC code: L01FF09). Tislelizumab is a humanised IgG4 variant monoclonal antibody that potentiates T-cell responses, including anti-tumour responses, through blockade of PD-1 binding to PD-L1 and PD-L2 ligands.The benefit of Tizveni is an improvement in overall survival and progression free survival in patients with locally advanced or metastatic NSCLC, as shown in three open-label, randomised phase 3 studies comparing Tizveni (either in monotherapy or in combination) with chemotherapy. The most common side effects are anaemia, fatigue and increased AST.The full indication is:Tizveni in combination with pemetrexed and platinum‑containing chemotherapy is indicated for the first-line treatment of adult patients with non-squamous non-small cell lung cancer whose tumours have PD-L1 expression on ≥50% of tumour cells with no EGFR or ALK positive mutations and who have:locally advanced NSCLC and are not candidates for surgical resection or platinum-based chemoradiation, ormetastatic NSCLC.Tizveni in combination with carboplatin and either paclitaxel or nab-paclitaxel is indicated for the first-line treatment of adult patients with squamous non-small cell lung cancer who have:locally advanced NSCLC and are not candidates for surgical resection or platinum-based chemoradiation, ormetastatic NSCLC.Tizveni as monotherapy is indicated for the treatment of adult patients with locally advanced or metastatic non-small cell lung cancer after prior platinum-based therapy. Patients with EGFR mutant or ALK positive NSCLC should also have received targeted therapies before receiving tislelizumab.Tizveni should be prescribed by physicians experienced in the treatment of cancer.Detailed recommendations for the use of this product will be described in the summary of product characteristics (SmPC), which will be published in the European public assessment report (EPAR) and made available in all official European Union languages after the marketing authorisation has been granted by the European Commission.CHMP summary of positive opinion for TizveniAdoptedFirst published: 23/02/2024Reference Number: EMA/CHMP/59203/2024 English (EN) (114.24 KB - PDF)ViewProduct detailsName of medicine Tizveni Active substance Tislelizumab International non-proprietary name (INN) or common name tislelizumab Therapeutic area (MeSH) Carcinoma, Non-Small-Cell Lung Anatomical therapeutic chemical (ATC) code L01FF09 EMA product number EMEA/H/C/005542 Marketing authorisation applicant BeiGene Ireland Ltd Opinion adopted 22/02/2024 Opinion status Positive This page was last updated on 23/02/2024Share this page
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Arnaud Delobel on LinkedIn: #cancertherapy #fdaapproval #tiltherapy #medicalinnovation…

Arnaud Delobel on LinkedIn: #cancertherapy #fdaapproval #tiltherapy #medicalinnovation… | Immunology and Biotherapies | Scoop.it
The FDA has just approved a revolutionary Tumor-Infiltrating Lymphocytes (TIL) therapy from Iovance Biotherapeutics, Inc.! But what exactly are TILs? 🤔

🔬…
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Jean Daniel Lelièvre sur LinkedIn : Webinaire vaccin grippe One Health 1 Oiseaux et hommes partage de…

Jean Daniel Lelièvre sur LinkedIn : Webinaire vaccin grippe One Health 1 Oiseaux et hommes partage de… | Immunology and Biotherapies | Scoop.it
Les présentations du "Webinaire vaccin anti grippe" One Health organisé par le DIM One Health 2.0 et le club de vaccinologie de la SFI sont désormais…
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Jeroen Wissink on LinkedIn: Cancer vaccines: the next immunotherapy frontier - Nature Cancer

Jeroen Wissink on LinkedIn: Cancer vaccines: the next immunotherapy frontier - Nature Cancer | Immunology and Biotherapies | Scoop.it
💥 How do we measure cancer vaccine immune responses? Is this similar to (simply..) measuring antibody titers, as in prophylactic vaccines? It took some time…
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https://www.nejm.org/doi/full/10.1056/NEJMoa2301790

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The antibody–drug conjugate renaissance

The antibody–drug conjugate renaissance | Immunology and Biotherapies | Scoop.it
Antibody–drug conjugates have emerged as a powerful tool to deliver highly targeted cancer therapies. Next-generation antibody-drug conjugate designs aim to push the envelope even further.
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Alexandre Loupy on LinkedIn: #xenotransplantation #paristransplantgroup #pitor #xenotransplant… | 17 comments

Alexandre Loupy on LinkedIn: #xenotransplantation #paristransplantgroup #pitor #xenotransplant… | 17 comments | Immunology and Biotherapies | Scoop.it
✨ Discovering New Horizons on #XENOTRANSPLANTATION ✨

We’re on an exhilarating journey to unravel the mysteries of xeno immune response. Our passion for… | 17 comments on LinkedIn
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ICOS costimulation in combination with CTLA-4 blockade remodels tumor-associated macrophages toward an antitumor phenotype | Journal of Experimental Medicine | Rockefeller University Press

The study unveils that potent combination therapies remodel TAMs to antitumor proinflammatory M1-like macrophages crucial for their therapeutic efficacy. I
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08 JAN 2024 — Future Vaccines — Medthority

08 JAN 2024 — Future Vaccines — Medthority | Immunology and Biotherapies | Scoop.it
The future of vaccine development in light of accelerated technological advances through the COVID-19 pandemic.
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Development of New Immunological Assays and Animal Models to Evaluate Vaccine Safety and Efficacy Against Emerging Diseases | FDA

Development of New Immunological Assays and Animal Models to Evaluate Vaccine Safety and Efficacy Against Emerging Diseases | FDA | Immunology and Biotherapies | Scoop.it
A description of H. Golding's research program and related publications.
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Immune targeting of HIV-1 reservoir cells: a path to elimination strategies and cure | Nature Reviews Microbiology

Immune targeting of HIV-1 reservoir cells: a path to elimination strategies and cure | Nature Reviews Microbiology | Immunology and Biotherapies | Scoop.it
Successful approaches for eradication or cure of HIV-1 infection are likely to include immunological mechanisms, but remarkably little is known about how human immune responses can recognize and interact with the few HIV-1-infected cells that harbour genome-intact viral DNA, persist long term despite antiretroviral therapy and represent the main barrier to a cure. For a long time regarded as being completely shielded from host immune responses due to viral latency, these cells do, on closer examination with single-cell analytic techniques, display discrete footprints of immune selection, implying that human immune responses may be able to effectively engage and target at least some of these cells. The failure to eliminate rebound-competent virally infected cells in the majority of persons likely reflects the evolution of a highly selected pool of reservoir cells that are effectively camouflaged from immune recognition or rely on sophisticated approaches for resisting immune-mediated killing. Understanding the fine-tuned interplay between host immune responses and viral reservoir cells will help to design improved interventions that exploit the immunological vulnerabilities of HIV-1 reservoir cells. Finding a cure for HIV-1 infection, once considered elusive, now represents a major priority for the global microbiology research community. In this article, Armani-Tourret, Lichterfeld and colleagues highlight recent advances in understanding immunological vulnerabilities of virally infected cells that persist lifelong and represent the major barrier to a cure.
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Natural killer cells lead the charge in cancer treatment innovation

Natural killer cells lead the charge in cancer treatment innovation | Immunology and Biotherapies | Scoop.it
Review synthesizes research on NK cells' role in cancer immunity and their potential in therapeutics through bioengineering, immune checkpoint inhibitors, and cell engagers, highlighting ongoing preclinical and clinical trials.

Via BigField GEG Tech
BigField GEG Tech's curator insight, March 4, 6:23 AM

In a recent study published in the journal Nature, researchers have compiled the available literature on natural killer (NK) cells, innate immune cells involved in the recognition and elimination of cells in distress, particularly virus-infected cells and tumors. They focus on reviewing current preclinical and clinical research in the field of NK therapies, primarily elucidating the role of NK cells in cancer immunity. They also explore the potential of bioengineering approaches to harness NK cells via the development of genetically modified NK cells, immune checkpoint inhibitors and cell engagement agents. The study reveals that, despite less than two decades of research in the field, NK cells are emerging as a safe, practical and potentially widely accessible means of clinical therapy, particularly antitumor. Although challenges exist in the adoption of NK cell therapies by conventional medicine, studies aimed at overcoming these challenges are already underway, bringing the future of clinical NK cell interventions closer than ever. 

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Sickle cell disease gene therapies Casgevy Lyfgenia insurance cost issues

Sickle cell disease gene therapies Casgevy Lyfgenia insurance cost issues | Immunology and Biotherapies | Scoop.it
Breakthrough sickle cell treatments are available in the U.S., but their high cost is forcing insurers to get creative.
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Powerful new antivenom raises hopes for a universal solution to lethal snakebites

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Bernard Maillere on LinkedIn: The target atlas for antibody-drug conjugates across solid cancers -…

Bernard Maillere on LinkedIn: The target atlas for antibody-drug conjugates across solid cancers -… | Immunology and Biotherapies | Scoop.it
interesting overview of the worldwide compétition for ADC. hard to find a place for a new product.
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COVID-19 and Flu-Ravaged Lungs Could Be Repaired with mRNA Therapy

COVID-19 and Flu-Ravaged Lungs Could Be Repaired with mRNA Therapy | Immunology and Biotherapies | Scoop.it

Repair of lung injury due to viral infection can be facilitated by nanoparticle-delivered mRNA targeting TGF-βR2 signaling. Respiratory infections, such as those caused by SARS-CoV-2 or influenza, can damage the lungs’ delicate network of capillary blood vessels, compromising oxygen delivery and carbon dioxide removal. To overcome this damage, the lungs depend on the regenerative capacities of vascular endothelial cells. As valuable as these cells are, they can, according to University of Pennsylvania scientists, benefit from a little help. The scientists, led by Andrew Vaughan, PhD, focused on a repair pathway involving vascular endothelial growth factor α (Vegfa) and the TGF-β receptor 2 (TGF-βR2). Using animal models and human tissue samples, the scientists showed that delivering Vegfa via lipid nanoparticles (LNPs) greatly enhances modes of repair for damaged blood vessels. “Mice deficient in endothelial Tgfbr2 exhibited prolonged injury and diminished vascular repair,” the article’s authors wrote. “Loss of endothelial Tgfbr2 prevented autocrine Vegfa expression, reduced endothelial proliferation, and impaired renewal of aerocytes thought to be critical for alveolar gas exchange.” “We developed a lipid nanoparticle that targets the pulmonary endothelium, Lung-LNP (LuLNP),” the authors continued. “Delivery of Vegfa mRNA, a critical TGF-βR2 downstream effector, by LuLNPs improved the impaired regeneration phenotype of endothelial cell Tgfbr2 deficiency during influenza injury.”

 

Vaughan’s team and other investigators had previously shown that endothelial cells are among the unsung heroes in repairing the lungs after viral infections. But Vaughan’s team noted that its work demonstrated that a “more granular understanding of the fundamental mechanisms driving reconstitution of lung endothelium” could inform efforts to facilitate therapeutic vascular repair. “Here we’ve identified and isolated pathways involved in repairing this tissue, delivered mRNA to endothelial cells, and consequently observed enhanced recovery of the damaged tissue,” Vaughan said. “These findings hint at a more efficient way to promote lung recovery after diseases like COVID-19.” The team found Vegfa’s involvement in this recovery, while building on work in which they used single-cell RNA sequencing to identify TGF-βR2 as a major signaling pathway. The researchers saw that when TGF-βR2 was missing, it stopped the activation of Vegfa. This lack of signal made the blood vessel cells less able to multiply and renew themselves, which is vital for the exchange of oxygen and carbon dioxide in the tiny air sacs of the lungs. “We’d known there was a link between these two pathways, but this motivated us to see if delivering Vegfa mRNA into endothelial cells could improve lung recovery after disease-related injury,” said first author Gan Zhao, PhD, a postdoctoral researcher in the Vaughan laboratory. The Vaughan laboratory then reached out to Michael J. Mitchell, PhD, of the School of Engineering and Applied Science, whose laboratory specializes in LNPs, to see if delivery of this mRNA cargo would be feasible.

 

“LNPs have been great for vaccine delivery and have proven incredibly effective delivery vehicles for genetic information,” said Mitchell, who is an associate professor of bioengineering at Penn Engineering and a co-author of the paper. “But the challenge here was to get the LNPs into the bloodstream without them heading to the liver, which is where they tend to congregate as its porous structure lends favor to substances passing from the blood into hepatic cells for filtration. So, we had to devise a way to specifically target the endothelial cells in the lungs.” The Mitchell laboratory’s LNPs proved effective in delivering Vegfa into endothelial cells, and as a result, the researchers saw a marked improvement in vascular recovery in their animal models. Within the animal models, the researchers saw improved oxygen levels, and in some, the treatment helped them recover their weight better than the control group. These treated mice also had less lung inflammation, shown by lower levels of certain markers in their lung fluid, and their lungs showed less damage and scarring, with more healthy blood vessels. “We’re looking forward to testing this delivery platform for other cell types in the lung, and it will be important to evaluate whether TGF-βR2 signaling is important in other injury contexts including chronic conditions like emphysema and chronic obstructive pulmonary disease,” Vaughan said. “With this proof-of-concept being well validated, we’re sure that we’ll pave the way for new mRNA-based strategies for treating lung injury.”

 

Published in January 31, 2024 in Science Translational Med:

https://doi.org/10.1126/scitranslmed.adg6229 


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Andrew Pannu sur LinkedIn : Is the best yet to come for cell therapy? I pulled together 45 companies… | 47 commentaires

Andrew Pannu sur LinkedIn : Is the best yet to come for cell therapy? I pulled together 45 companies… | 47 commentaires | Immunology and Biotherapies | Scoop.it
Is the best yet to come for cell therapy?

I pulled together 45 companies in the space and charted the preclinical and clinical assets of each, segmented by… | 47 commentaires sur LinkedIn
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Immunotherapeutic targeting of activating natural killer cell receptors and their ligands in cancer | Clinical and Experimental Immunology | Oxford Academic

Immunotherapeutic targeting of activating natural killer cell receptors and their ligands in cancer | Clinical and Experimental Immunology | Oxford Academic | Immunology and Biotherapies | Scoop.it
Natural Killer (NK) cells exert an important role in cancer immune surveillance and recognition of malignant cells as well as their controlled activation is fac
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