Design, Synthesis and Phenotypic Profiling of Simplified Gedatolisib Analogues

Costa, Caroline Marques Xavier; Aparecida-Silva, Cristiane; Gamba, Luis Eduardo Reina; Melo, Thalita Neves de; Barbosa, Gisele; Moraes, Manoel Oliveira de; Oliveira, Victoria Regina Thomaz de; Amorim, Carolinne Souza; Moraes, João Alfredo; Barreiro, Eliezer J.; Lima, Lı́dia Moreira

doi:10.3390/ph16020209

Cited by 4 publications

(2 citation statements)

References 28 publications

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“…Considering the cell viability studies in the MTT of 72 h, gedatolisib displayed average cytotoxic concentration (CC 50 ) values of 0.86 µM, 70 nM, 90 nM and 60 nM to PC-3, MOLT-4, CCRF-CEM and MCF-7, respectively. These results are similar to the values of 0.54 µM, 20 nM, 30 nM e 70 nM, respectively, previously described by Costa et al [ 12 ] in regard to the performance of gedatolisib against the same tumour cell lines ( Table 1 ). It is worth noting that our work is the first to describe the cytotoxic effect of gedatolisib in 24 h and 48 h MTT assays on PC-3 and MCF-7 tumour cell lines.…”

Section: Resultssupporting

confidence: 92%

Cytotoxic and Antiproliferative Activity of LASSBio-2208 and the Attempts to Determine Its Drug Metabolism and Pharmacokinetics In Vitro Profile

Pillpe-Meza,

Gouveia,

Barbosa

et al. 2024

Pharmaceuticals

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Inappropriate expression of histone deacetylase (HDAC-6) and deregulation of the phosphatidylinositol 3-kinase (PI3K) signalling pathway are common aberrations observed in cancers. LASSBio-2208, has been previously described as a dual inhibitor in the nanomolar range of HDAC-6 and PI3Kα and is three times more potent in inhibiting HDAC-6. In this paper we described the cytotoxic and antiproliferative potency of LASSBio-2208 on different tumour cell lines, its possible synergism effect in association with PI3K and HDAC-6 inhibitors, and its drug metabolism and pharmacokinetics (DMPK) in vitro profile. Our studies have demonstrated that LASSBio-2208 has moderate cytotoxic potency on breast cancer cell line MCF-7 (IC50 = 23 µM), human leukaemia cell line CCRF-CEM (IC50 = 8.54 µM) and T lymphoblast cell line MOLT-4 (IC50 = 7.15 µM), with no cytotoxic effect on human peripheral blood mononuclear cells (hPBMC). In addition, it has a good antiproliferative effect on MCF-7 cells (IC50 = 5.44 µM), low absorption by parallel artificial membrane permeability—gastrointestinal tract (PAMPA—GIT) and low permeation by parallel artificial membrane permeability—blood–brain barrier (BBB) (PAMPA—BBB), exhibiting high metabolic stability in rat plasma. Moreover, LASSBio-2208 exhibited synergism when combined with getadolisib and tubastatin A, using the concentrations corresponding to their CC50 values on MOLT-4 and CCRF-CEM cells.

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Section: Resultssupporting

confidence: 92%

Cytotoxic and Antiproliferative Activity of LASSBio-2208 and the Attempts to Determine Its Drug Metabolism and Pharmacokinetics In Vitro Profile

Pillpe-Meza,

Gouveia,

Barbosa

et al. 2024

Pharmaceuticals

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“…This new analog has great aqueous solubility and high metabolic stability in rat liver microsomes. Taken together, LASSBio‐2252 (5f) can be considered a new lead candidate, whose structural optimization is required to increase its cytotoxic potency (Costa et al, 2023).…”

Section: Introductionmentioning

confidence: 99%

Method development and validation for the estimation of gedatolisib in mouse plasma by tandem mass spectrometry and its application to pharmacokinetics studies

A B,

Das

2024

Biomedical Chromatography

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A simple and a sensitive liquid chromatography–tandem mass spectrometry method was developed and validated for the quantification of gedatolisib in mouse plasma. The extraction technique involved a simple precipitation method to extract gedatolisib and idelalisib (internal standard) from mouse plasma. A clean chromatographic separation of gedatolisib and the internal standard was achieved on an Atlantis dC18 column using an isocratic mobile phase (10 mm ammonium formate and acetonitrile; 30:70% v/v, both supplemented with 0.1% formic acid) delivered at a flow rate of 0.7 ml/min. The total run time was 2.0 min, and gedatolisib and idelalisib were eluted at 0.80 and 0.95 min, respectively. Gedatolisib was monitored at m/z 616.40 → 488.20 and idelalisib at 416.05 → 176.10. All the required parameters for the method validation were performed as per US Food and Drug Administration guidelines, and the results were within the acceptance criteria. The method was accurate and proved to be precise at a linearity range of 1.33–2667 ng/ml. The accuracy for gedatolisib in mouse plasma was in the ranges 0.99–1.06% (intra‐day) and 0.96–1.04% (inter‐day). Gedatolisib appeared to be stable in a series of stability conditions. Gedatolisib showed a good intravenous profile when administered through a solution formulation.

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