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A fundus image of a healthy retina.
Ocular

Novel inducible mouse model of North Carolina macular dystrophy

Feb. 20, 2024
At the recent Macula Society Meeting, researchers from the Molecular Insight Research Foundation reported on the creation of a novel murine model of North Carolina macular dystrophy.
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CAR T cell attacking cancer cells
Immuno-oncology

STING agonist IMSA-101 improves CAR T therapy trafficking into tumor

Feb. 20, 2024
Immunesensor Therapeutics Inc. has presented preclinical data on the stimulator of interferon genes (STING) agonist IMSA-101 which is designed to modify the tumor microenvironment in solid tumors and thus improve the trafficking and infiltration of CAR T-cell therapy into the tumor.
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DNA illustration
Endocrine/Metabolic

Gene therapy with AAV2/8-LSPhGAA shows good results in preclinical Pompe disease

Feb. 19, 2024
Pompe disease is a disorder caused by deficiency of the lysosomal acid α-glucosidase (GAA) enzyme, which leads to the accumulation of glycogen within the lysosomes, overall in skeletal and cardiac muscle.
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Endocrine/Metabolic

GCS inhibitor YH-35995A ameliorates Gaucher disease in mice

Feb. 19, 2024
Yuhan Corp. has presented preclinical data on their glucosylceramide synthase (GCS) inhibitor.
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Cross section of brainstem
Infection

AAAS 2024: Chemo brain, other conditions provide lens for long COVID

Feb. 19, 2024
By Nuala Moran
The biological processes giving rise to the central nervous system symptoms of long COVID remain a mystery. But multiple studies suggest they do not appear to be a result of a direct viral infection of brain tissue. The latest such research, which appeared online in Nature Neuroscience on Feb. 16, 2024, demonstrated that local immune response in brain tissues persisted long after SARS-CoV-2 virus had disappeared.
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Drug R&D concept image.
Endocrine/Metabolic

Pompe disease murine model harboring GAA c.1826dupA resembles infantile-onset disease

Feb. 16, 2024
Pompe disease is caused by a deficiency in the lysosomal enzyme acid α-glucosidase (GAA) that leads to accumulation of glycogen in the lysosomes, mainly seen in skeletal and cardiac muscles. Researchers from Duke University have developed a new murine model of Pompe disease, which recapitulates human infantile-onset disease. This model harbors the c.1826dupA mutation in the murine Gaa gene, which resembles the human GAA c.1826dupA (p.Y609*) mutation seen in infantile-onset Pompe disease.
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Neurology/Psychiatric

New mouse model of COVID-19-induced cerebrovascular embolic complications

Feb. 15, 2024
Researchers from Mercer University have presented a middle cerebral artery/ferric chloride (MCA/FeCl3) thromboembolic mouse model of COVID-19-induced stroke and cerebrovascular complications.
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A lysosome (foreground) is enlarged by an accumulation of the fatty substance glucocerebroside, a characteristic of Gaucher disease
Endocrine/Metabolic

Murine model recapitulates human Gaucher disease type 1

Feb. 15, 2024
Researchers from the Yale University School of Medicine have developed a novel murine model of Gaucher disease type I with the aim to investigate the impact of GBA1 deficiency on hematopoiesis and the immune system, in order to elucidate potential therapeutic targets.
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Endocrine/Metabolic

Autologous B-cell therapy WFX-001 corrects systemic α-GAL enzyme deficiency in vivo

Feb. 14, 2024
Walking Fish Therapeutics Inc. presented a new first-in-class autologous B-cell therapy being developed for the treatment of Fabry disease.
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Neurology/Psychiatric

VST Bio presents data on novel anti-syndecan-2 antibody

Feb. 14, 2024
It has been shown that vascular endothelial growth factor A (VEGF-A) induces blood-brain barrier disruption and vasogenic edema and it is up-regulated in stroke. When bound to its receptor, VEGF promotes angiogenesis and neuroprotection, in addition to inducing vasogenic edema. VST Bio Ltd. and Yale University have presented data on their monoclonal antibody against syndecan-2, named VST-002, that completely blocks VEGF-driven vasogenic edema while preserving neuroprotective effects.
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