A novel adjuvant drug-device combination tissue scaffold for radical prostatectomy

Paliashvili, Ketevan; Maggio, Francesco; Ho, Hei Ming Kenneth; Sathasivam, Sanjayan; Ahmed, Hashim U.; Day, Richard M.

doi:10.1080/10717544.2019.1686085

Cited by 5 publications

(13 citation statements)

References 39 publications

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“…Furthermore, since the TIPS process is highly versatile, the method used to produce films in the current study provides scope to produce polymer films that exhibit different roughness and pore structures via adjustment of parameters including the polymer:solvent ratio, composition of PLGA (ratio of lactide to glycolide), solvent, and rate of quenching. [ 27 ] The ability to control these parameters through further refinement of the porous films provides greater opportunity to fine tune the proangiogenic effect achieved compared with other approaches investigated for therapeutic angiogenesis, such as gene‐based therapy, thus lowering concerns over oncogenic risks. This provides scope for future studies aimed at elucidating optimal properties of the porous polymer films for regulating therapeutic angiogenesis.…”

Section: Resultsmentioning

confidence: 99%

Microporous Biodegradable Films Promote Therapeutic Angiogenesis

Hendow

Moazen

Iacoviello

et al. 2020

Adv Healthcare Materials

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Peripheral arterial disease and critical limb ischemia are common symptoms of cardiovascular disease. Vascular surgery is used to create a bypass around occluded blood vessels to improve blood flow to ischemic muscle, thus avoiding the need for amputation. Attempts to vascularize tissues by therapeutic angiogenesis using delivery of exogenous angiogenic agents are underwhelming. A material‐based approach that provides an endogenous stimulus capable of promoting angiogenesis and increased tissue perfusion would provide a paradigm shift in treatment options available. It is reported here that microporous biodegradable films produced using thermally induced phase separation provide a localized biophysical stimulus of proangiogenic genes in vivo that is associated with increased blood vessel density and restoration of blood flow to ischemic tissue. These findings show, for the first time, that acellular, nonfunctionalized biodegradable biomaterials can provide an innovative, material‐based approach for therapeutic angiogenesis to enhance tissue reperfusion in vivo.

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Section: Resultsmentioning

confidence: 99%

Microporous Biodegradable Films Promote Therapeutic Angiogenesis

Hendow

Moazen

Iacoviello

et al. 2020

Adv Healthcare Materials

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“…7,10,11 The TIPS method not only permits tailoring of microparticle size (from nano-to microscale in diameter), porosity and pore morphology but also allows inclusion of active ingredients such as small molecules and protein based therapies into the polymer matrix, as well providing a delivery vehicle for advanced therapies. 8,[11][12][13][14] A further beneficial attribute of PLGA polymeric microparticles is their compatibility with a wide range of materials, including synthetic polymers 15 and biological materials such as antibodies, enabling targeting of specific disease biomarkers. 16 To date, most of the loading of active ingredients such as antibodies or small molecules into micro/nanoparticle systems has been achieved by either blending the compounds into the polymer solution during the fabrication process 11,12,16 or using post-fabrication random conjugation methods (electrostatic or covalent) to append the two entities, e.g.…”

Section: Introductionmentioning

confidence: 99%

“…physisorption or covalently attaching antibodies (via random surface lysine residue modification) to particles via carbodiimide chemistry. 14,17,18 However, in the case of loading microparticles with antibody, the aforementioned procedures greatly limit antigen-binding and overall target avidity, as well making it difficult to control aggregation. We have recently demonstrated the importance of controlled chemical "click" ligation of proteins for successful nanoconjugate performance, particularly in the context of target affinity.…”

Section: Introductionmentioning

confidence: 99%

“… 7 , 10 , 11 The TIPS method not only permits tailoring of microparticle size (from nano- to micro-scale in diameter), porosity and pore morphology but also allows inclusion of active ingredients such as small molecules and protein based therapies into the polymer matrix, as well providing a delivery vehicle for advanced therapies. 8 , 11 – 14 …”

Section: Introductionmentioning

confidence: 99%

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Functionalised thermally induced phase separation (TIPS) microparticles enabled for “click” chemistry

et al. 2020

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“…[13] Given the accessibility of residual cancer in the prostate bed or tissue cavity due to positive surgical margins following excision of the prostate, we have previously proposed the use of biodegradable microparticles to enable the targeted delivery of DTX as an adjuvant therapy during surgical removal of the prostate for cancer. [14] Our previous study established an optimized process for loading TIPS microparticles with DTX and demonstrated in vitro their potential utility for tumor growth inhibition over a period of 12 days. The antisolvent precipitation method used for loading TIPS microparticles with DTX differs from other methods used in previous drug-delivery studies with TIPS microparticles and results in drug being predominantly coated onto the microsphere surface.…”

Section: Introductionmentioning

confidence: 99%

Peritumoral Delivery of Docetaxel‐TIPS Microparticles for Prostate Cancer Adjuvant Therapy

Paliashvili

Popov

Kalber

et al. 2020

Advanced Therapeutics

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Recurrence of prostate cancer after radical prostatectomy is a consequence of incomplete tumor resection. Systemic chemotherapy after surgery is associated with significant toxicity. Improved delivery methods for toxic drugs capable of targeting positive resection margins can reduce tumor recurrence and avoid their known toxicity. This study evaluates the effectiveness and toxicity of docetaxel (DTX) release from highly porous biodegradable microparticles intended for delivery into the tissue cavity created during radical prostatectomy to target residual tumor cells. The microparticles, composed of poly(dl-lactide-co-glycolide) (PLGA), are processed using thermally induced phase separation (TIPS) and loaded with DTX via antisolvent precipitation. Sustained drug release and effective toxicity in vitro are observed against PC3 human prostate cells. Peritumoral injection in a PC3 xenograft tumor model results in tumor growth inhibition equivalent to that achieved with intravenous delivery of DTX. Unlike intravenous delivery of DTX, implantation of DTX-TIPS microparticles is not accompanied by toxicity or elevated systemic levels of DTX in organ tissues or plasma. DTX-TIPS microparticles provide localized and sustained release of nontoxic therapeutic amounts of DTX. This may offer novel therapeutic strategies for improving management of patients with clinically localized high-risk disease requiring radical prostatectomy and other solid cancers at high risk of positive resection margins.

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A novel adjuvant drug-device combination tissue scaffold for radical prostatectomy

Cited by 5 publications

References 39 publications

Microporous Biodegradable Films Promote Therapeutic Angiogenesis

Microporous Biodegradable Films Promote Therapeutic Angiogenesis

Functionalised thermally induced phase separation (TIPS) microparticles enabled for “click” chemistry

Peritumoral Delivery of Docetaxel‐TIPS Microparticles for Prostate Cancer Adjuvant Therapy

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