Phase I/II Clinical Trial of Encapsulated, Cytochrome P450 Expressing Cells as Local Activators of Cyclophosphamide to Treat Spontaneous Canine Tumours

Michałowska, Monika; Winiarczyk, S.; Adaszek, Łukasz; Łopuszyński, Wojciech; Grądzki, Z.; Salmons, Brian; Günzburg, Walter H.

doi:10.1371/journal.pone.0102061

Cited by 8 publications

(11 citation statements)

References 32 publications

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“…We have performed a clinical trial in dogs using encapsulated cells to locally activate this chemotherapeutic after peritumoral injection [ 8 , 51 , 52 ]. Tumor reductions were also observed in this clinical trial in companion animals [ 52 ], supporting the notion that the mechanism of action is not due to a simple obstruction of the blood vessels leading to the tumor, since in this study, the capsules were administered by injection directly into the tissues round the tumor site. Further, CT-scans taken during and after angiography in our human pancreatic cancer trials showed the patency of the vessels after instillation of the capsules.…”

Section: Discussionmentioning

confidence: 99%

Encapsulated Cells Expressing a Chemotherapeutic Activating Enzyme Allow the Targeting of Subtoxic Chemotherapy and Are Safe and Efficacious: Data from Two Clinical Trials in Pancreatic Cancer

et al. 2014

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Despite progress in the treatment of pancreatic cancer, there is still a need for improved therapies. In this manuscript, we report clinical experience with a new therapy for the treatment of pancreatic cancer involving the implantation of encapsulated cells over-expressing a cytochrome P450 enzyme followed by subsequent low-dose ifosfamide administrations as a means to target activated ifosfamide to the tumor. The safety and efficacy of the angiographic instillation of encapsulated allogeneic cells overexpressing cytochrome P450 in combination with low-dose systemic ifosfamide administration has now been evaluated in 27 patients in total. These patients were successfully treated in four centers by three different interventional radiologists, arguing strongly that the treatment can be successfully used in different centers. The safety of the intra-arterial delivery of the capsules and the lack of evidence that the patients developed an inflammatory or immune response to the encapsulated cells or encapsulation material was shown in all 27 patients. The ifosfamide dose of 1 g/m2/day used in the first trial was well tolerated by all patients. In contrast, the ifosfamide dose of 2 g/m2/day used in the second trial was poorly tolerated in most patients. Since the median survival in the first trial was 40 weeks and only 33 weeks in the second trial, this strongly suggests that there is no survival benefit to increasing the dose of ifosfamide, and indeed, a lower dose is beneficial for quality of life and the lack of side effects. This is supported by the one-year survival rate in the first trial being 38%, whilst that in the second trial was only 23%. However, taking the data from both trials together, a total of nine of the 27 patients were alive after one year, and two of these nine patients were alive for two years or more.

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Section: Discussionmentioning

confidence: 99%

Encapsulated Cells Expressing a Chemotherapeutic Activating Enzyme Allow the Targeting of Subtoxic Chemotherapy and Are Safe and Efficacious: Data from Two Clinical Trials in Pancreatic Cancer

et al. 2014

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“…Additionally, their handling in the lab does not represent any complications and can be treated as cells and be frozen without damage. Importantly, the use of cellulose sulphate encapsulated human cells is safe in patients as has been demonstrated in two human clinical trials (Löhr et al, 2014) and in a veterinary application (Michałowska et al, 2014).…”

Section: Introductionmentioning

confidence: 94%

“…Cell encapsulation is a classic technique that has been applied for the delivery of active therapeutic agents from entrapped cells (Acarregui et al, 2013;Gonzalez-Pujana et al, 2017). Their application ranges from insulin release therapy for type 1 diabetes (Orlando et al, 2014) to other life-threatening pathologies, such as cancer (Löhr et al, 2014;Michałowska et al, 2014); also, capsules in general represent the possibility of their localization in a desired area (Dangerfield et al, 2013). The capsule structure must be permeable in order to enable nutrients and waste flux but also the release of the therapeutic agent(s).…”

Section: Introductionmentioning

confidence: 99%

Semipermeable Cellulose Beads Allow Selective and Continuous Release of Small Extracellular Vesicles (sEV) From Encapsulated Cells

et al. 2020

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Here, we successfully present a novel, cost, and time-saving method to generate sEV from encapsulated MSCs. Future applications include using encapsulated cells as a retrievable delivery device that can interact with the host niche by releasing active agents in vivo, including sEV, growth factors, hormones, and small molecules, while avoiding cell clearance, and the negative side-effect of releasing undesired components including apoptotic bodies. Finally, particles produced following the encapsulation protocol display beneficial features for their use as drug-loaded delivery vehicles.

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“…CMT, the same as human breast cancer (BC), can be characterized by expression of estrogen, progesterone and HER2 receptors. The involvement of companion dogs with spontaneous CMT in translational oncology is already seen in numerous publications and several ongoing clinical trials (13). Canine tumoroids developed from dog patients with spontaneous CMT could therefore provide a more representative and ethical translational model to test drug efficacy and toxicity in pre-human studies, as well as canine tumoroids could be an innovative screening tool in drug discovery, while reducing the number of experimental animals needed for in vivo studies.…”

Section: Introductionmentioning

confidence: 99%

Establishment and characterization of a tumoroid biobank derived from dog patients’ mammary tumors for translational research

Raffo-Romero

Aboulouard

Bouchaert

et al. 2022

Preprint

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Breast cancer is the most frequent cancer among women causing the greatest number of cancer-related deaths. Cancer heterogeneity is a main obstacle to therapies. Around 96% of the drugs fail from discovery to the clinical trial phase probably because of the current unreliable preclinical models. New models emerge such as companion dogs who develop spontaneous mammary tumors resembling human breast cancer in many clinical and molecular aspects. The present work aimed at developing a robust canine mammary tumor model in the form of tumoroids which recapitulate the tumor diversity and heterogeneity. We conducted a complete characterization of these canine mammary tumoroids through histologic, molecular and proteomic analysis, demonstrating their strong similarity to the primary tumor. We demonstrated that these tumoroids can be used as a drug screening model. In fact, we showed that Paclitaxel, a human chemotherapeutic, could killed canine tumoroids with the same efficacy as human tumoroids with 0.1 to 1 μM of drug needed to kill 50% of the cells. Due to easy tissue availability, canine tumoroids can be produced at larger scale and cryopreserved to constitute a biobank. We have demonstrated that cryopreserved tumoroids keep the same histologic and molecular features (ER, PR and HER2 expression) as fresh tumoroids. Two techniques of cryopreservation were compared demonstrating that tumoroids made from frozen tumor material allowed to maintain a higher molecular diversity. These findings revealed that canine mammary tumoroids can be easily generated at large scale and can represent a more reliable preclinical model to investigate tumorigenesis mechanisms and develop new treatments for both veterinary and human medicine.

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Phase I/II Clinical Trial of Encapsulated, Cytochrome P450 Expressing Cells as Local Activators of Cyclophosphamide to Treat Spontaneous Canine Tumours

Cited by 8 publications

References 32 publications

Encapsulated Cells Expressing a Chemotherapeutic Activating Enzyme Allow the Targeting of Subtoxic Chemotherapy and Are Safe and Efficacious: Data from Two Clinical Trials in Pancreatic Cancer

Encapsulated Cells Expressing a Chemotherapeutic Activating Enzyme Allow the Targeting of Subtoxic Chemotherapy and Are Safe and Efficacious: Data from Two Clinical Trials in Pancreatic Cancer

Semipermeable Cellulose Beads Allow Selective and Continuous Release of Small Extracellular Vesicles (sEV) From Encapsulated Cells

Establishment and characterization of a tumoroid biobank derived from dog patients’ mammary tumors for translational research

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