Amikacin in 30% poloxamer 407 is a versatile local therapy with method of application and outcome documented in 29 dogs

Risselada, Marije; Spies, Kate E.; Kim, Sun Young

doi:10.2460/javma.24.01.0048

Cited by 2 publications

References 23 publications

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In vitroefficacy andin vivotoxicity and retention of targeted nanoformulated carboplatin in a sustained release carrier for treatment of osteosarcoma

Day,

Risselada,

Sokolsky-Papkov

2024

Preprint

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Objective: evaluate 1) if targeting of platinum nagnetic nanoclusters will promote uptake in osteosarcoma cells in vitro, 2) targeting will improve uptake and delivery in murine OSA in vivo compared to free carboplatin, 3) incorporation into a sustained release carrier (SRC) will prolong local retention in vivo. Methods: Complex stability and peptide loading was assessed. Drug release was tested at pH 7.4 and 5.5 and cellular uptake and cytotoxity determined for canine, human and mouse osteosarcoma. Subcutaneous murine osteosarcoma was induced and optimal dose and time until tumor growth were established. Tumor bearing mice were equally distributed between 8 treatment (0.5mg carboplatin/mouse) and 1 control group and sacrificed at 8 predetermined time points between 1 hour and 8 days. Blood, tumor site and organs were harvested for tissue ferron and platinum content analysis (ICP-MS). Results: Carboplatin was preferentially released at pH5.5. Targeting increased cellular uptake for carboplatin 15.2-fold, and decreased IC50 at 24h and 48h. At 2 weeks, a SC injection of 1-1.56 live cells/mouse reliably resulted in a palpable tumor. Plasma platinum peaked prior to 6 hours while plasma ferron peaked at 24-48 hours. Intratumoral delivery did not lead to a sustained local presence while local delivery in a SRC after surgery did. Conclusions: Targeting of MNC-carboplatin fis possible with an increased osteosarcoma cell uptake in vitro. In vivo metastatic uptake could not be assessed due to lack of metastases, but local delivery in a SRC yielded high local, and low systemic platinum concentrations in mice.

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In vitroefficacy andin vivotoxicity and retention of targeted nanoformulated carboplatin in a sustained release carrier for treatment of osteosarcoma

Day,

Risselada,

Sokolsky-Papkov

2024

Preprint

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Silver nanoparticles can be sampled by ultrafiltration probe but elution into & recovery from plasma and Dulbecco’s Phosphate Buffered Saline differs in vitro

Risselada,

McCain,

Bates

et al. 2024

PeerJ

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Locally sustained release antimicrobials such as silver nanoparticles (AgNPs) might prove useful in combating local infections. Their elution has been investigated in Phosphate Buffered Saline (PBS) including from poloxamer 407 (P407). No information exists on possible interactions with proteins, nor have ultrafiltration (UF) probes been evaluated to measure Ag. These investigations would provide helpful data prior to investigating the sustained release after subcutaneous implantation in vivo over time. We compared (1) the influence of elution fluid on AgNP elution, and (2) UF probe and direct sampling in vitro. Six AgNP-P407 specimens in a dialysis tube were placed in Dulbecco’s PPBS (DPBS) (n = 3) or canine plasma (n = 3) for 96 h on a stirred hot plate (37 °C and 600 rpm) and sampled 20 times. A 0.001 mg/mL AgNP solution was prepared in DPBS or plasma. Six pipette and UF probe samples were taken of each. Inductively coupled plasma mass spectrometry was used to analyze Ag. Stock plasma contained Ag. At 96 h, 5/6 dialysis tubes had not fully released AgNP. One peak in hourly Ag increase was present in DPBS (10–13 h), and two peaks in plasma (6–8 and 10–13 h). The hourly Ag increase in plasma decreased earlier than in DPBS. Ultrafiltration probe sampling was possible in both DPBS and plasma and resulted in higher Ag concentrations but with more variation. While in vitro use of DPBS might be more cost effective, plasma should be considered due to difference in elution and recovery. Ultrafiltration probes can be used to sample Ag, but results will have a greater degree of variation, and multiple samples and increased time points should be considered.

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Amikacin in 30% poloxamer 407 is a versatile local therapy with method of application and outcome documented in 29 dogs

Cited by 2 publications

References 23 publications

In vitroefficacy andin vivotoxicity and retention of targeted nanoformulated carboplatin in a sustained release carrier for treatment of osteosarcoma

In vitroefficacy andin vivotoxicity and retention of targeted nanoformulated carboplatin in a sustained release carrier for treatment of osteosarcoma

Silver nanoparticles can be sampled by ultrafiltration probe but elution into & recovery from plasma and Dulbecco’s Phosphate Buffered Saline differs in vitro

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