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BioWorld - Monday, May 25, 2026
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Sunrise in a desert with sand dunes
Inflammatory

Study gives insight into five inflammatory diseases, and the noncoding genome

June 25, 2024
By Anette Breindl
A recent paper has identified the enhancer ETS2, located in a so-called gene desert, as a contributor to five separate immune disorders. It also showed that one of ETS2’s target genes mediating this inflammation was the eminently druggable MEK, a kinase that is the target of the FDA-approved inhibitors Mekinist (trametinib, GSK plc), Mektovi (binimetinib, Array Biopharma Inc.), Cotellic (cobimetinib, Roche Holding AG) and Koselugo (selumetinib, Astrazeneca plc/Merck & Co. Inc.).
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Cancer

SSO-110-based radiopharmaceuticals more efficacious against SST2 receptor-positive tumors

June 21, 2024
SSO-110, also known as DOTA-JR11 or satoreotide tetraxetran, is a somatostatin SST2 receptor (SSTR2) antagonist that targets a higher number of binding sites and stays longer in SSTR2-positive tumors compared to SST2 receptor agonists. It is currently in clinical development as [177Lu]Lu-SSO-110 for small-cell lung cancer (SCLC). Ariceum Therapeutics GmbH has revealed preclinical data on [177Lu]Lu-SSO-110 as well as another SSO-110-based radiopharmaceutical, [225Ac]Ac-SSO-110, which yielded better results than DOTA-TATE-conjugated isotopes.
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Hepatitis B virus
Infection

Novel CAM-A candidates show rapid HBsAg reductions in vivo

June 21, 2024
Aligos Therapeutics Inc. have discovered two novel non-heteroaryldihydropyrimidine (HAP) class A capsid assembly modulators (CAM-A) – ALG-006746 and ALG-006780 – which are being developed for the treatment of hepatitis B virus (HBV) infection.
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Hematologic

Potential first-in-class agent for JAK2 V617F mutant myeloproliferative neoplasms

June 21, 2024
Researchers from Incyte Corp. and collaborators presented the preclinical profile of INCB-160058, an ATP-competitive small-molecule inhibitor of the JAK2 V617F mutant sparing its wild-type (WT) form, designed for the treatment of JAC2 V617F mutation-positive myeloproliferative neoplasms with potential as a first-in-class JAK2 V617-inhibiting drug.
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Cancer

Astrazeneca’s first-in-class T-cell engager circumvents associated toxicities

June 21, 2024
Bispecific CD20×CD3 T-cell engagers have shown efficacy in hematological malignancies; however, associated toxicities such as cytokine release syndrome and immune effector-associated neurotoxicity syndrome limit their use.
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Bladder cancer illustration
Cancer

RUVBL1/2 inhibitor CB-6644 promotes cell cycle arrest in bladder cancer

June 20, 2024
Bladder cancer is characterized by a high recurrence rate, with limited therapeutic options available. There is a need to discover new therapeutic targets and approaches to overcome this.
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Antibody-drug conjugate illustration
Cancer

New anti-TIM-3 antibody-drug conjugate displays efficacy in AML models

June 20, 2024
Residual leukemic stem cells (LSCs) are leukemia relapse-initiating cells that mediate treatment resistance in response to therapy stress. Different from normal hematopoietic stem cells (HSCs), both blasts and LSCs express T-cell immunoglobulin mucin-3 (TIM-3) on the surface.
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Cancer

Anticancer quinolone yields antileukemia effects and overcomes venetoclax resistance

June 20, 2024
Targeting topoisomerase 2 (TOP2) is crucial in AML, and researchers from Wakunaga Pharmaceutical Co. Ltd. have developed and tested racemic WAC-224, a quinolone TOP2 inhibitor, and (R)-WAC-224 as a potential approach for AML treatment.
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Lab glassware and scientist
Diagnostics

[68Ga]LW-02050, GRPR-targeted PET tracer with low hepatobiliary excretion and reduced pancreas uptake

June 20, 2024
Researchers from BC Cancer Research Institute (Provincial Health Services Authority) and the University of British Columbia have presented the discovery and preclinical characterization of [68Ga]LW-02050, a 68Ga-labeled hydroxamate derivative of SB3.
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Hematologic

Incyte’s anti-CALR displays robust antimyeloproliferative effect

June 20, 2024
Among the acquired mutations in the calreticulin (CALR) gene, both 52 bp deletion (del52) and 5 bp insertion (ins5) are among the most frequent and are linked to two different types of myeloproliferative neoplasms (MPNs).
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