A Phase 1 Trial of Oncolytic Adenovirus ICOVIR-5 Administered Intravenously to Cutaneous and Uveal Melanoma Patients

García, Margarita; Moreno, Rafael; Gil-Martín, Marta; Cascalló, Manel; Olza, María Ochoa de; Cuadra, C.; Piulats, Josep María; Navarro, V.; Doménech, Marta; Alemany, Ramón; Salazar, Ramón

doi:10.1089/hum.2018.107

Cited by 75 publications

(57 citation statements)

References 30 publications

(50 reference statements)

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“…Second, the highly efficient binding of coagulation FX of human origin to HAdv-C5 was also shown for mouse coagulation FX [8]. Sixth and last, leukocytopenia and thrombocytopenia observed after intravenous administration of HAdv to mice [] are also observed in rabbits [150], nonhuman primates [59], and humans [148] but not in pigs [151]. Fourth, the cytosolic inactivation of HAdv-Ab complexes by TRIM21 appears to function in both mouse and human systems [141,142].…”

Section: Complexity Of Designing Hadv Vectors With Reduced Innate Immmentioning

confidence: 93%

“…First, HAdv serotypes of species A, C, D, E, and F can utilize CAR of both human and mouse origin as a primary high-affinity attachment receptor to gain entry into human and mouse cells [39,40]. Fifth, high-dose intravenous delivery to mice [143] and nonhuman primates [59] of HAdv triggers an acute release of IL-6 and TNF-a, a response stereotypically observed in patients with severe natural HAdv infection [144][145][146] and during clinical gene therapy trials with systemic delivery of high doses of HAdv-based vectors [60,147,148]. Third, the natural IgM-and complement-mediated inactivation of FX-binding-ablated HAdv-C5-based vectors occurs in both mouse and human sera [26,27].…”

Section: Complexity Of Designing Hadv Vectors With Reduced Innate Immmentioning

confidence: 99%

“…Fourth, the cytosolic inactivation of HAdv-Ab complexes by TRIM21 appears to function in both mouse and human systems [141,142]. Fifth, high-dose intravenous delivery to mice [143] and nonhuman primates [59] of HAdv triggers an acute release of IL-6 and TNF-a, a response stereotypically observed in patients with severe natural HAdv infection [144][145][146] and during clinical gene therapy trials with systemic delivery of high doses of HAdv-based vectors [60,147,148]. Sixth and last, leukocytopenia and thrombocytopenia observed after intravenous administration of HAdv to mice [] are also observed in rabbits [150], nonhuman primates [59], and humans [148] but not in pigs [151].…”

Section: Relevance Of Mice and Other Animals As Models Of Human Immunmentioning

confidence: 99%

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Innate immunity to adenovirus: lessons from mice

2019

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Adenovirus is a highly evolutionary successful pathogen, as it is widely prevalent across the animal kingdom, infecting hosts ranging from lizards and frogs to dolphins, birds, and humans. Although natural adenovirus infections in humans rarely cause severe pathology, intravenous injection of high doses of adenovirus-based vectors triggers rapid activation of the innate immune system, leading to cytokine storm syndrome, disseminated intravascular coagulation, thrombocytopenia, and hepatotoxicity, which individually or in combination may cause morbidity and mortality. Much of the information on exactly how adenovirus activates the innate immune system has been gathered from mouse experimental systems. Intravenous administration of adenovirus to mice revealed mechanistic insights into cellular and molecular components of the innate immunity that detect adenovirus particles, activate pro-inflammatory signaling pathways and cytokine production, sequester adenovirus particles from the bloodstream, and eliminate adenovirus-infected cells. Collectively, this information greatly improved our understanding of mechanisms of activation of innate immunity to adenovirus and may pave the way for designing safer adenovirus-based vectors for therapy of genetic and acquired human diseases.Human adenovirus (HAdv) is remarkably efficient at infecting and replicating in human cells. These properties made HAdv-based vectors an attractive platform for developing novel therapeutics to combat genetic diseases and cancer. Unfortunately, early studies revealed that HAdv is a potent activator of the innate and adaptive arms of the immune system, and administration to animals or patients of high doses of HAdv-based vectors, especially via an intravascular route, leads to severe immunopathology, manifested by cytokine storm syndrome, disseminated intravascular coagulation, thrombocytopenia, and hepatotoxicity, which may lead to morbidity and even mortality. To harness the full potential of HAdv as a gene delivery or oncolytic virus platform, a complete understanding of the molecular and cellular components of innate Abbreviations is a founder, shareholder, and chief scientific officer of AdCure Bio, LLC, which develops Ad-based therapies for clinical use.

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Section: Complexity Of Designing Hadv Vectors With Reduced Innate Immmentioning

confidence: 93%

Section: Complexity Of Designing Hadv Vectors With Reduced Innate Immmentioning

confidence: 99%

Section: Relevance Of Mice and Other Animals As Models Of Human Immunmentioning

confidence: 99%

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Innate immunity to adenovirus: lessons from mice

2019

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“…in clinical trials (44,77,(87)(88)(89). In addition, oncolytic adenovirus caused pleural effusion, dehydration, hypokalemia, severe liver dysfunction, and sepsis in clinical trials (90)(91)(92). Severe hematological abnormalities (leukopenia, lymphopenia, and neutropenia), hypokalemia and pancreatitis were observed in the trials of oncolytic pox virus (93)(94)(95)(96).…”

Section: Biosafety Of Oncolytic Virotherapy Adverse Events Induced Bymentioning

confidence: 99%

Delivery and Biosafety of Oncolytic Virotherapy

et al. 2020

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In recent years, oncolytic virotherapy has emerged as a promising anticancer therapy. Oncolytic viruses destroy cancer cells, without damaging normal tissues, through virus self-replication and antitumor immunity responses, showing great potential for cancer treatment. However, the clinical guidelines for administering oncolytic virotherapy remain unclear. Delivery routes for oncolytic virotherapy to patients vary in existing studies, depending on the tumor sites and the objective of studies. Moreover, the biosafety of oncolytic virotherapy, including mainly uncontrolled adverse events and long-term complications, remains a serious concern that needs to be accurately measured. This review provides a comprehensive and detailed overview of the delivery and biosafety of oncolytic virotherapy.

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“…Replication-selective oncolytic adenoviruses (OAds) with these modifications, such as CV706, CG7870, AdD24RGD, and ICOVIR5, entered clinical trials. However, despite occasional striking tumor responses, clinical efficacy remained low [7][8][9][10][11]. Thus, the potency of oncolytic adenoviruses should be further increased…”

Section: Introductionmentioning

confidence: 99%

Effect of Transgene Location, Transcriptional Control Elements and Transgene Features in Armed Oncolytic Adenoviruses

Farrera-Sal

Fillat

Alemany

2020

Cancers

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Clinical results with oncolytic adenoviruses (OAds) used as antitumor monotherapies show limited efficacy. To increase OAd potency, transgenes have been inserted into their genome, a strategy known as "arming OAds". Here, we review different parameters that affect the outcome of armed OAds. Recombinant adenovirus used in gene therapy and vaccination have been the basis for the design of armed OAds. Hence, early region 1 (E1) and early region 3 (E3) have been the most commonly used transgene insertion sites, along with partially or complete E3 deletions. Besides transgene location and orientation, transcriptional control elements, transgene function, either virocentric or immunocentric, and even the codons encoding it, greatly impact on transgene levels and virus fitness.

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A Phase 1 Trial of Oncolytic Adenovirus ICOVIR-5 Administered Intravenously to Cutaneous and Uveal Melanoma Patients

Cited by 75 publications

References 30 publications

Innate immunity to adenovirus: lessons from mice

Innate immunity to adenovirus: lessons from mice

Delivery and Biosafety of Oncolytic Virotherapy

Effect of Transgene Location, Transcriptional Control Elements and Transgene Features in Armed Oncolytic Adenoviruses

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