Multistep, effective drug distribution within solid tumors

Shemi, Amotz; Khvalevsky, Elina Zorde; Gabai, Rachel Malka; Domb, Abraham J.; Barenholz, Yechezkel

doi:10.18632/oncotarget.5051

Cited by 26 publications

(15 citation statements)

References 54 publications

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“…This result is not surprising due to the lake of the lymph vasculature in the tumor compared to the normal tissue. The trend of the results agrees well with the previous studies in the literature 1,27,28 .…”

Section: Resultssupporting

confidence: 92%

“…Cancer is one of the most dangerous and deadliest diseases that cause deaths of millions of people around the world each year. More than 85% of human cancers appear as solid tumors 1 . Minimally invasive and image-guided thermal ablation techniques such as radiofrequency ablation (RFA) and high-intensity focused ultrasound (HIFU) ablation have been used for local treatment of malignant solid tumors as an alternative for systemic chemotherapy and surgical resection 2 .…”

Section: Introductionmentioning

confidence: 99%

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Modelling of combination therapy using implantable anticancer drug delivery with thermal ablation in solid tumor

Al-Zu'bi

Mohan

2020

Sci Rep

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Local implantable drug delivery system (IDDS) can be used as an effective adjunctive therapy for solid tumor following thermal ablation for destroying the residual cancer cells and preventing the tumor recurrence. In this paper, we develop comprehensive mathematical pharmacokinetic/pharmacodynamic (PK/PD) models for combination therapy using implantable drug delivery system following thermal ablation inside solid tumors with the help of molecular communication paradigm. In this model, doxorubicin (DOX)-loaded implant (act as a transmitter) is assumed to be inserted inside solid tumor (acts as a channel) after thermal ablation. Using this model, we can predict the extracellular and intracellular concentration of both free and bound drugs. Also, Impact of the anticancer drug on both cancer and normal cells is evaluated using a pharmacodynamic (PD) model that depends on both the spatiotemporal intracellular concentration as well as characteristics of anticancer drug and cells. Accuracy and validity of the proposed drug transport model is verified with published experimental data in the literature. The results show that this combination therapy results in high therapeutic efficacy with negligible toxicity effect on the normal tissue. The proposed model can help in optimize development of this combination treatment for solid tumors, particularly, the design parameters of the implant.

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Section: Resultssupporting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Modelling of combination therapy using implantable anticancer drug delivery with thermal ablation in solid tumor

Al-Zu'bi

Mohan

2020

Sci Rep

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“…Or the implants established a sharp zone of drug gradient near the surrounding tissue, and drop very quickly further away from the surface of the implant [16] [18]. Or the pharmacokinetic measurements will be vastly different from the systemic administrated route in other possibilities [21]. Yet this leads to another striking question: during those 21 days, close to 700 mcg of doxorubicin was released from the implant, twice that of the IV group.…”

Section: Low Plasma Doxorubicin Of the Stid100 Implant Correlated Witmentioning

confidence: 99%

“…Drug exposure in this manner leads to higher resistance and is yet another way tumor cells to escape. Placement of a solid chemotherapy implant within or near the tumor mass might address this dilemma [21].…”

Section: Introductionmentioning

confidence: 99%

A Totally Absorbable Multilayer PLGA Implant Device Containing Doxorubicin Inhibited Tumor Growth and Metastasis without Systemic Toxicity in Murine Breast Cancer and an Ideal Pharmacological Paradigm for Regional Chemotherapy

Elzey¹,

Torregrosa-Allen²,

Li³

et al. 2016

JBM

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We hypothesize that a cylinder implant made of multilayer Poly-lactic-co-glycolic-acid (PLGA) membrane can be a method for controlled and extended drug release. We fashioned a multilayer cylindrical implant termed STID100 that released doxorubicin for 3 weeks in an orthotopic 4T1 breast cancer model in Balb/C mice. This implant starts as a thin doxorubicin-embedded PLGA membrane, and is then rolled into a cylinder containing an air gap between the membrane layers. Its controlled sustained release delivered 2× the amount of the intravenous (IV) equivalent of doxorubicin, inhibited the primary tumor, and prevented lung metastasis. Importantly it did not cause weight loss, splenomegaly, or cardiac toxicity vs systemically administrated doxorubicin. This favorable safety profile is further substantiated by the finding of no detectable plasma doxorubicin in multiple time points during the 3-week period, and low tumor doxorubicin concentration. The implant system delivered to the specification of an ideal pharmacological paradigm might offer a better coverage of the local tumor, significantly preventing metastatic spread with less drug toxicity to many vital organs, compared to the traditional pharmacology of IV route. The profile of STID made it an attractive therapeutic alternative in metastatic tumor prevention, pain management * Corresponding author. B. Elzey et al. 67and many other diverse clinical scenarios.

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“…Development of methods to avoid this limitation is an important challenge in medical oncology. Strategies that have been assessed to address this challenge in the last decades include: combination therapies aimed at improving tumor vascularization or reducing IFP 32 , 33 , development of drugs that selectively target hypoxic regions 34 , and the use of devices that allow a controlled and continuous release of therapeutic drugs 35 . All these strategies, when successful, result in a significant increase of necrotic/apoptotic cell death throughout the entire tumor parenchyma, thus indicating the successful delivery of therapeutic drugs in regions that are normally inaccessible.…”

Section: Discussionmentioning

confidence: 99%

Theranostic Role of ³²P-ATP as Radiopharmaceutical for the Induction of Massive Cell Death within Avascular Tumor Core

et al. 2017

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Drug inaccessibility to vast areas of the tumor parenchyma is amongst the major hurdles for conventional therapies. Treatment efficacy rapidly decreases with distance from vessels and most of the tumor cells survive therapy. Also, between subsequent cycles of treatment, spared cancer cells replace those killed near the vessels, improving their access to nutrients, boosting their proliferation rate, and thus enabling tumor repopulation. Because of their property of "acting at a distance," radioisotopes are believed to overcome the physical barrier of vascular inaccessibility.Methods A novel molecular imaging tool called Cerenkov Luminescence Imaging (CLI) was employed for the detection of Cerenkov radiation emitted by beta particles, allowing in vivo tracking of beta-emitters. More precisely we investigated using a xenograft model of colon carcinoma the potential use of 32P-ATP as a novel theranostic radiopharmaceutical for tracing tumor lesions while simultaneously hampering their growth.Results Our analyses demonstrated that 32P-ATP injected into tumor-bearing mice reaches tumor lesions and persists for days and weeks within the tumor parenchyma. Also, the high-penetrating beta particles of 32P-ATP exert a "cross-fire" effect that induces massive cell death throughout the entire tumor parenchyma including core regions.Conclusion Our findings suggest 32P-ATP treatment as a potential approach to complement conventional therapies that fail to reach the tumor core and to prevent tumor repopulation.

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Multistep, effective drug distribution within solid tumors

Cited by 26 publications

References 54 publications

Modelling of combination therapy using implantable anticancer drug delivery with thermal ablation in solid tumor

Modelling of combination therapy using implantable anticancer drug delivery with thermal ablation in solid tumor

A Totally Absorbable Multilayer PLGA Implant Device Containing Doxorubicin Inhibited Tumor Growth and Metastasis without Systemic Toxicity in Murine Breast Cancer and an Ideal Pharmacological Paradigm for Regional Chemotherapy

Theranostic Role of ³²P-ATP as Radiopharmaceutical for the Induction of Massive Cell Death within Avascular Tumor Core

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Multistep, effective drug distribution within solid tumors

Cited by 26 publications

References 54 publications

Modelling of combination therapy using implantable anticancer drug delivery with thermal ablation in solid tumor

Modelling of combination therapy using implantable anticancer drug delivery with thermal ablation in solid tumor

A Totally Absorbable Multilayer PLGA Implant Device Containing Doxorubicin Inhibited Tumor Growth and Metastasis without Systemic Toxicity in Murine Breast Cancer and an Ideal Pharmacological Paradigm for Regional Chemotherapy

Theranostic Role of 32P-ATP as Radiopharmaceutical for the Induction of Massive Cell Death within Avascular Tumor Core

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Theranostic Role of ³²P-ATP as Radiopharmaceutical for the Induction of Massive Cell Death within Avascular Tumor Core