Sustained, low-dose intraperitoneal cisplatin improves treatment outcome in ovarian cancer mouse models

Ye, Hongye; Tanenbaum, Laura M.; Na, Young Jeong; Mantzavinou, Aikaterini; Fulci, Giulia; Carmen, Marcela G. del; Birrer, Michael J.; Cima, Michael J.

doi:10.1016/j.jconrel.2015.11.001

Cited by 15 publications

(10 citation statements)

References 33 publications

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“…An implantable, nonresorbable IP micro-device was developed to release a chemotherapeutic agent to the peritoneal cavity at a constant rate. 10 Preclinical studies showed reduced toxicity by the controlled drug release from this micro-device with similar efficacy outcomes to frequent IP bolus doses. Current efforts related to IP drug delivery are mainly to provide a depot for sustained release of chemotherapeutic agents in the peritoneal tumor environment, thus increasing local drug levels while reducing systemic exposure.…”

mentioning

confidence: 79%

Improving paclitaxel pharmacokinetics by using tumor-specific mesoporous silica nanoparticles with intraperitoneal delivery

Hargrove

Lü

2016

Nanomedicine: Nanotechnology, Biology and Medicine

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Mesoporous silica nanoparticles (MSNs) containing paclitaxel for intraperitoneal (i.p.) delivery were developed to exploit the tumor specific accumulation of these nanocarriers after i.p. injection and the slow release of paclitaxel from the MSNs. A 3.5-fold increase in tumor cellular drug uptake was observed for the paclitaxel-loaded MSNs compared with free paclitaxel. An in vivo study using xenograft mice bearing peritoneal human pancreatic carcinoma MIA PaCa-2 demonstrated that the MSN-paclitaxel formulation, compared to free paclitaxel, exhibited a 3.2-fold increase in peritoneal cavity residence time, slower absorption into the systemic circulation with one third systemic exposure, but a 6.5-fold increase in peritoneal tumor accumulation. Tissue distribution imaging showed significantly greater accumulation of fluorescent MSNs in tumor tissues compared to other peritoneal tissues. In conclusion, intraperitoneal administration of drug-containing MSNs was effective at reducing systemic exposure and increasing the peritoneal tumor accumulation of paclitaxel.

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mentioning

confidence: 79%

Improving paclitaxel pharmacokinetics by using tumor-specific mesoporous silica nanoparticles with intraperitoneal delivery

Hargrove

Lü

2016

Nanomedicine: Nanotechnology, Biology and Medicine

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“…Additionally, the work by Colin et al [36] does estimate the changes in tumour volume based on a PDPD link suggested by Ait-Oudhia et al [65]. Given the recent interest in metronomic chemotherapy in the context of IP chemotherapy [66], extending models to include growth and cell survival might become more frequent.…”

Section: Discussionmentioning

confidence: 99%

Modelling drug transport during intraperitoneal chemotherapy

Steuperaert

Debbaut

Segers

et al. 2017

Pleura and Peritoneum

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Despite a strong rationale for intraperitoneal (IP) chemotherapy, the actual use of the procedure is limited by the poor penetration depth of the drug into the tissue. Drug penetration into solid tumours is a complex mass transport process that involves multiple parameters not only related to the used cytotoxic agent but also to the tumour tissue properties and even the therapeutic setup. Mathematical modelling can provide unique insights into the different transport barriers that occur during IP chemotherapy as well as offer the possibility to test different protocols or drugs without the need for in vivo experiments. In this work, a distinction is made between three different types of model: the lumped parameter model, the distributed model and the cell-based model. For each model, we discuss which steps of the transport process are included and where assumptions are made. Finally, we focus on the advantages and main limitations of each category and discuss some future perspectives for the modelling of IP chemotherapy.

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“…who developed a delivery device for IP administration of cisplatin. [ 155 ] The device design was based on in vitro work by the group that demonstrated that sustained low doses of cisplatin produced better killing of ovarian cancer cells than intermittent dosing. [ 156 ] The devices used were fabricated from poly‐ l ‐lactic acid and consisted of a spherical chamber and cap.…”

Section: Advanced Delivery Solutionsmentioning

confidence: 99%

“…The cap had a circular orifice with a diameter of 180 μm, chosen to control cisplatin release based on its solubility and diffusivity. [ 155 ] The devices were loaded with 5 mg cisplatin powder. The device was tested in mice, using weekly IP bolus injections (5 mg kg −1 ) as a control.…”

Section: Advanced Delivery Solutionsmentioning

confidence: 99%

“…The device released cisplatin continuously over 42 days with an approximate release rate of 1 μg h −1 . [ 155 ] Both IP injection and cisplatin delivery using the device significantly reduced tumor burden compared to the untreated control. There was no significant difference in tumor mass or tumor burden between the IP bolus injection and microdevice groups.…”

Section: Advanced Delivery Solutionsmentioning

confidence: 99%

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Enhancing Delivery of Small‐Molecule‐ and Cell‐Based Therapies for Ovarian Cancer Using Advanced Delivery Strategies

O’Dwyer

O’Cearbhaill

Wylie

et al. 2020

Advanced Therapeutics

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Ovarian cancer is the most lethal gynecological malignancy with a global five‐year survival rate of 30–50%. First‐line treatment involves cytoreductive surgery and administration of platinum‐based small molecules and paclitaxel. These therapies are traditionally administered via intravenous infusion, although intraperitoneal delivery has also been investigated. Initial clinical trials of intraperitoneal administration for ovarian cancer indicate significant improvements in overall survival compared to intravenous delivery, but this result is not consistent across all studies performed. Recently, cell‐based immunotherapy has been of interest for ovarian cancer. Direct intraperitoneal delivery of cell‐based immunotherapies may prompt local immunoregulatory mechanisms to act synergistically with the delivered immunotherapy. Based on this theory, preclinical in vivo studies have delivered these cell‐based immunotherapies via the intraperitoneal route, with promising results. However, successful intraperitoneal delivery of cell‐based immunotherapy and clinical adoption of this technique depend on overcoming challenges of intraperitoneal delivery and finding the optimal combinations of dose, therapeutic, and delivery route. The potential advantages and disadvantages of intraperitoneal delivery of cell‐based immunotherapy for ovarian cancer and the preclinical and clinical work performed so far are reviewed. Potential advanced delivery strategies, which may improve the efficacy and adoption of intraperitoneal delivery of therapy for ovarian cancer, are also outlined.

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Sustained, low-dose intraperitoneal cisplatin improves treatment outcome in ovarian cancer mouse models

Cited by 15 publications

References 33 publications

Improving paclitaxel pharmacokinetics by using tumor-specific mesoporous silica nanoparticles with intraperitoneal delivery

Improving paclitaxel pharmacokinetics by using tumor-specific mesoporous silica nanoparticles with intraperitoneal delivery

Modelling drug transport during intraperitoneal chemotherapy

Enhancing Delivery of Small‐Molecule‐ and Cell‐Based Therapies for Ovarian Cancer Using Advanced Delivery Strategies

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