Author: Zunarelli, Renato ; Fiore, Michele ; Sambri, Andrea ; Cappelli, Alberta ; Bruschi, Alessandro ; Scollo, Cristina ; Di Prinzio, Lorenzo ; Montanari, Andrea ; Pace, Andrea ; Bubbico, Elisa ; De Paolis, Massimiliano

ABSTRACT:

Introduction:

Bone metastases and pathological fractures significantly impact the prognosis and quality of life in cancer patients. However, clinical and radiological features alone have been shown to fail to predict skeletal related events of a bone metastasis (SREs).

Aim:

This study focuses on key molecular players including Matrix Metalloproteinases (MMPs), Integrins, Bone Morphogenetic Proteins (BMPs), Parathormone‐related Protein (PTHrP).

Results:

The RANK/RANKL/Osteoprotegerin (OPG) pathway, and N‐terminal peptide (NTx), involved in the metastatic process and bone integrity disruption. Elevated levels of these molecules have been pointed out as potential biomarkers for predicting SREs, but they have been poorly investigated. Moreover, batimastat, marimastat, tanomastat, andecaliximab, and HIV protease targeting MMPs; Volociximab/M200, cilengitide, abituzumab, and FAK inhibitors targeting integrins; LDN193189, DMH1, and ISLR modulators targeting BMPs; and PTH (7–33)‐CBD targeting PTHrP have shown promising results antagonizing these molecules, but no effect on preventing and managing metastatic fractures has been assessed yet.

Conclusions:

This paper underscores the importance of advanced molecular biology and transcriptomics in identifying novel therapeutic targets. The integration of these biomarkers with clinical and radiological assessments using artificial intelligence tools could revolutionize the diagnostics and treatment strategies for patients with bone metastases.

01 Dec 2024·CELLULAR AND MOLECULAR LIFE SCIENCES

Identification of novel neuroprotectants against vincristine-induced neurotoxicity in iPSC-derived neurons

Article

Author: Cheng, Anya ; Snavely, Andrew R ; Singh, Bhagat ; Splaine, Jennifer ; Woolf, Clifford J ; Barrett, Lee B ; Petrova, Veselina ; Hermawan, Crystal ; Chen, Kuchuan ; Zhen, Shannon ; Pandey, Roshan ; Smith, Jennifer A

Abstract:

Chemotherapy-induced peripheral neuropathy (CIPN) is a disabling side effect of cancer chemotherapy that can often limit treatment options for cancer patients or have life-long neurodegenerative consequences that reduce the patient’s quality of life. CIPN is caused by the detrimental actions of various chemotherapeutic agents on peripheral axons. Currently, there are no approved preventative measures or treatment options for CIPN, highlighting the need for the discovery of novel therapeutics and improving our understanding of disease mechanisms. In this study, we utilized human-induced pluripotent stem cell (hiPSC)-derived motor neurons as a platform to mimic axonal damage after treatment with vincristine, a chemotherapeutic used for the treatment of breast cancers, osteosarcomas, and leukemia. We screened a total of 1902 small molecules for neuroprotective properties in rescuing vincristine-induced axon growth deficits. From our primary screen, we identified 38 hit compounds that were subjected to secondary dose response screens. Six compounds showed favorable pharmacological profiles – AZD7762, A-674563, Blebbistatin, Glesatinib, KW-2449, and Pelitinib, all novel neuroprotectants against vincristine toxicity to neurons. In addition, four of these six compounds also showed efficacy against vincristine-induced growth arrest in human iPSC-derived sensory neurons. In this study, we utilized high-throughput screening of a large library of compounds in a therapeutically relevant assay. We identified several novel compounds that are efficacious in protecting different neuronal subtypes from the toxicity induced by a common chemotherapeutic agent, vincristine which could have therapeutic potential in the clinic.

01 Sep 2024·DRUG DEVELOPMENT RESEARCH

Biphenylsulfonamides as effective MMP‐2 inhibitors with promising antileukemic efficacy: Synthesis, in vitro biological evaluation, molecular docking, and MD simulation analysis

Article

Author: Das, Sanjib ; Adhikari, Nilanjan ; Ghosh, Balaram ; Patel, Tarun ; Banerjee, Suvankar ; Jha, Tarun ; Himaja, Ambati ; Baidya, Sandip K.

Abstract:

Overexpression of matrix metalloproteinase‐2 (MMP‐2) possesses a correlation with leukemia especially chronic myeloid leukemia (CML). However, no such MMP‐2 inhibitor has come out in the market to date for treating leukemia. In this study, synthesis, biological evaluation, and molecular modeling studies of a set of biphenylsulfonamide derivatives as promising MMP‐2 inhibitors were performed, focusing on their potential applications as antileukemic therapeutics. Compounds DH‐18 and DH‐19 exerted the most effective MMP‐2 inhibition (IC50 of 139.45 nM and 115.16 nM, respectively) with potent antileukemic efficacy against the CML cell line K562 (IC50 of 0.338 µM and 0.398 µM, respectively). The lead molecules DH‐18 and DH‐19 reduced the MMP‐2 expression by 21.3% and 17.8%, respectively with effective apoptotic induction (45.4% and 39.8%, respectively) in the K562 cell line. Moreover, both these compounds significantly arrested different phases of the cell cycle. Again, both these molecules depicted promising antiangiogenic efficacy in the ACHN cell line. Nevertheless, the molecular docking and molecular dynamics (MD) simulation studies revealed that DH‐18 formed strong bidentate chelation with the catalytic Zn2+ ion through the hydroxamate zinc binding group (ZBG). Apart from that, the MD simulation study also disclosed stable binding interactions of DH‐18 and MMP‐2 along with crucial interactions with active site amino acid residues namely His120, Glu121, His124, His130, Pro140, and Tyr142. In a nutshell, this study highlighted the importance of biphenylsulfonamide‐based novel and promising MMP‐2 inhibitors to open up a new avenue for potential therapy against CML.

News (Medical) associated with Batimastat

18 Apr 2023

·www.biospace.com

Affimed Shares Preclinical Data on AFM13’s Mechanism of Action Demonstrating Its Potential to Induce Serial Killing at the American Association for Cancer Research Annual Meeting

The poster presentation highlights the relevance of CD16A shedding for serial killing by AFM13-engaged natural killer (NK) cells It demonstrates the potential of AFM13 to induce serial killing, even in tumor cells with low target expression HEIDELBERG, Germany, April 17, 2023 (GLOBE NEWSWIRE) -- Affimed N.V. (Nasdaq: AFMD), a clinical-stage immuno-oncology company committed to giving patients back their innate ability to fight cancer, today presented a poster developed in collaboration with Prof. Björn Önfelt from the KTH Royal Institute of Technology and Karolinska Institute in Stockholm. The preclinical data demonstrate the ability of AFM13, Affimed’s CD16A/CD30-targeting innate cell engager (ICE®), to induce serial killing of tumor cells, while preserving CD16A shedding. The poster, shown at the Annual Meeting of the American Association for Cancer Research (AACR) in Orlando, Florida, shared results from a live-cell microchip screening with single cell resolution. AFM13 increased NK killing efficiency of CD30-positive tumor cells via antibody-dependent cellular cytotoxicity (ADCC). For CD30 high-expressing targets, AFM13 and an anti-CD30 Fc-enhanced antibody triggered higher NK cell-mediated ADCC and serial killing than a monoclonal anti-CD30 antibody. However, for CD30 low-expressing tumor cells, AFM13 induced significantly stronger serial killing compared to both the monoclonal anti-CD30 antibody and the Fc-enhanced anti-CD30 antibody, which led to significantly higher cytotoxicity against the target cells. In addition, the simultaneous administration of the CD16A shedding inhibitor Batimastat and AFM13 did not reduce the fraction of tumor-cell killing NK cells, but did reduce their ability to kill in series. With Batimastat, the fraction of NK cells performing at least one kill did not change, but significantly more NK cells died after their first killing. It was shown that more NK cells were stuck to target cells, when CD16A shedding was inhibited, and that they spent more time in conjugation. This leads to the hypothesis that CD16A shedding allows the NK cells to migrate to distantly located target cells after their first killing to proceed with additional AFM13-induced ADCC. However, after CD16A shedding inhibition, NK cells could still move around, dragging their target cells with them. “AFM13 increased NK cell-mediated serial killing of tumor cells, even when they express low levels of CD30,” said Prof. Björn Önfelt. “And CD16A shedding seems to facilitate the migration of AFM13-armed NK cells to distant target cells.” “It is impressive to see AFM13-engaged NK cells migrating at single cell resolution,” said Arndt Schottelius, chief scientific officer of Affimed. “With Prof. Önfelt’s microchip technology we can follow AFM13-engaged NK cells to see how they kill several tumor cells in sequence. This opens up new opportunities to gain a deeper understanding of their mechanism of action.” Pre-complexed with cord blood-derived NK cells, AFM13 has already yielded very compelling clinical data in a Phase 1/2a study. Affimed is now on track to submit the IND for a Phase 2 combination study of AFM13 co-administered with NK cells in the first half of 2023. The presented poster can be found on Affimed’s website at . About AFM13 AFM13 is a first-in-class tetravalent bispecific innate cell engager (ICE®) that uniquely activates the innate immune system to destroy CD30-positive hematologic tumors. AFM13 induces specific and selective killing of CD30-positive tumor cells, leveraging the power of the innate immune system by engaging and activating natural killer (NK) cells and macrophages. AFM13 is Affimed’s most advanced ICE® clinical program and was evaluated as monotherapy in a phase 2 trial in patients with relapsed/refractory peripheral T-cell lymphoma (REDIRECT, NCT04101331). Additional details can be found . In addition, The University of Texas MD Anderson Cancer Center is studying AFM13 in an investigator-sponsored Phase 1 trial in combination with cord blood-derived allogeneic NK cells in patients with recurrent or refractory CD30-positive lymphomas (NCT04074746). About Affimed N.V. Affimed (Nasdaq: AFMD) is a clinical-stage immuno-oncology company committed to give patients back their innate ability to fight cancer by actualizing the untapped potential of the innate immune system. The company’s proprietary ROCK® platform enables a tumor-targeted approach to recognize and kill a range of hematologic and solid tumors, enabling a broad pipeline of wholly-owned and partnered single agent and combination therapy programs. The ROCK® platform predictably generates customized innate cell engager (ICE®) molecules, which use patients’ immune cells to destroy tumor cells. This innovative approach enabled Affimed to become the first company with a clinical-stage ICE®. Headquartered in Heidelberg, Germany, with offices in New York, NY, Affimed is led by an experienced team of biotechnology and pharmaceutical leaders united by a bold vision to stop cancer from ever derailing patients’ lives. For more about the company’s people, pipeline and partners, please visit: . Investor Relations Contact Alexander Fudukidis Director, Investor Relations E-Mail: a.fudukidis@affimed.com Tel.: +1 (917) 436-8102 Media Contact Mary Beth Sandin Vice President, Marketing and Communications E-Mail: m.sandin@affimed.com

Phase 2ImmunotherapyAACR

100 Deals associated with Batimastat

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KEGG	Wiki	ATC	Drug Bank
D03061	Batimastat	-	DB03880

R&D Status

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Indication	Highest Phase	Country/Location	Organization	Date
Ascites	Phase 3	-	BTG International Ltd.	-
Ascites	Phase 3	-	InSite Vision, Inc.	-
Ascites	Phase 3	-	Ligand UK Ltd.	-

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


SFN2000	Not Applicable	Thromboembolic stroke TNF-alpha	-	BB-94	xtklchwfzb(uitlhmwklj) = pyagagytos jnvzqfqoar (kyvixfgpwe )	Positive	06 Nov 2000
				tPA	xtklchwfzb(uitlhmwklj) = gknsdpabze jnvzqfqoar (kyvixfgpwe )

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