Safety and efficacy of p62 DNA vaccine ELENAGEN in a first-in-human trial in patients with advanced solid tumors

Пономаренко, Д. М.; Клімова, Ірина; Chapygina, Yulia A.; Дворниченко, В. В.; Zhukova, Natalia V.; Орлова, Р. В.; Manikhas, Georgy M.; Zyryanov, Alexandr V.; Бурханова, Л А; Badrtdinova, Irina I.; Oshchepkov, Basile N.; Филиппова, Елена; Орлов, С. В.; Kolesnikov, S. I.; Sufianov, Albert; Baum, Svetlana R.; Zaitzeva, Olga Y.; Komissarov, Andrey; Грудинин, М П; Киселев, О. И.; Цыб, А. Ф.; Venanzi, Franco; Shcherbinina, Vita; Chursov, Andrey; Gabai, Vladimir L.; Shneider, Alexander

doi:10.18632/oncotarget.16574

Cited by 25 publications

(32 citation statements)

References 47 publications

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“…osteosarcoma, oral squamous cell carcinoma, cutaneous malignant melanoma, esophageal adenocarcinoma, ovarian, colon, breast and non-small cell lung cancers, and solid tumors Daniels et al, 2013;Ellis et al, 2014;Giatromanolaki et al, 2014;Inoue et al, 2012;Iwadate et al, 2014;Liu et al, 2014a;Luo et al, 2013;Ma et al, 2018;Niklaus et al, 2017;Park et al, 2013;Ruan et al, 2018;Schläfli et al, 2016), and has attracted attention as a potential therapeutic target (Yan et al, 2017;Zhang et al, 2016). An antitumor SQSTM1 DNA vaccine has already been developed and trialed in humans (Gabai et al, 2014;Ponomarenko et al, 2017;Sabbieti et al, 2015;Venanzi et al, 2013); however, SQSTM1 can have both beneficial and deleterious effects depending on the pathological context, as is the case for autophagy itself (Dikic and Elazar, 2018). Then, any hope to develop successful therapeutic strategies in pathologies with SQSTM1 alterations needs to keep in mind the complexity of the SQSTM1 signaling network and how it is affected in each particular disease situation: its tight posttranslational regulation, its role in autophagy, its function in the Keap1-Nrf2 axis and its role as a signaling hub.…”

Section: Discussionmentioning

confidence: 99%

p62/SQSTM1 – steering the cell through health and disease

Sánchez‐Martín

Komatsu

2018

Journal of Cell Science

218

179

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SQSTM1 (also known as p62) is a multifunctional stress-inducible scaffold protein involved in diverse cellular processes. Its functions are tightly regulated through an extensive pattern of post-translational modifications, and include the isolation of cargos degraded by autophagy, induction of the antioxidant response by the Keap1-Nrf2 system, as well as the regulation of endosomal trafficking, apoptosis and inflammation. Accordingly, malfunction of SQSTM1 is associated with a wide range of diseases, including bone and muscle disorders, neurodegenerative and metabolic diseases, and multiple forms of cancer. In this Review, we summarize current knowledge regarding regulation, post-translational modifications and functions of SQSTM1, as well as how they are dysregulated in various pathogenic contexts.

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Section: Discussionmentioning

confidence: 99%

p62/SQSTM1 – steering the cell through health and disease

Sánchez‐Martín

Komatsu

2018

Journal of Cell Science

218

179

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“…On the other hand, encouraging results were recently reported about a clinical trial of AdCD40L gene therapy combined with cyclophosphamide chemotherapy for human melanoma[31] and p62 protein (SQSTM1) gene therapy for some human solid tumors[32]. These trials were respectively based on previous veterinary trials involving canine melanoma[33] and canine mammary adenocarcinoma[22] patients.…”

Section: Resultsmentioning

confidence: 99%

Recent clinical trials of cancer immunogene therapy in companion animals

Finocchiaro

Glikin

2017

WJEM

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This mini-review presents the results of veterinary clinical trials on immunogene therapy published from 2014 to 2016. A variety of tumors, among them melanoma (canine and equine), mastocytoma (canine), mammary adenocarcinoma (canine) and fibrosarcoma (feline) were treated by using diverse strategies. Non-viral vectors were usually employed to transfer genes of cytokines, suicide enzymes and/or tumor associated antigens. In general terms, minor or no adverse collateral effects were related to these procedures, and treated patients frequently improved their conditions (better quality of life, delayed or suppressed recurrence or metastatic spread, increased survival). Some of these new methodologies have a promising future if applied as adjuvant treatments of standard approaches. The auspicious results, derived from immunogene therapy studies carried out in companion animals, warrant their imperative usage in veterinary clinical oncology. Besides, they provide a strong preclinical basis (safety assays and proofs of concept) for analogous human clinical trials.

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“…Safety and efficacy of p62 DNA injections has been further evaluated in a first‐in‐human trial in patients with advanced solid tumours . Of note p62 DNA treatment of patients partially restored their sensitivity to conventional chemotherapy which they previously failed . However, it remains to be revealed if the anti‐cancer activity of p62‐encoding plasmid in humans is due to a direct adaptive immune response it elicits against the over‐expressed p62 as it was originally hypothesized or if the anti‐cancer effect results from the fact that the plasmid reduces chronic inflammation as observed in animal models for osteoporosis, age‐related macular degeneration and diet‐induced obesity .…”

Section: Discussionmentioning

confidence: 98%

“…The observed anti‐tumour activity was associated with (CD3 + ) T cell infiltration and tumour encapsulation via fibrotic reaction. Safety and efficacy of p62 DNA injections has been further evaluated in a first‐in‐human trial in patients with advanced solid tumours . Of note p62 DNA treatment of patients partially restored their sensitivity to conventional chemotherapy which they previously failed .…”

Section: Discussionmentioning

confidence: 99%

p62/SQSTM1 expression in canine mammary tumours: Evolutionary notes

Mariotti

Magi

Gavazza

et al. 2019

Vet Comparative Oncology

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Recent studies highlighted the role of autophagy as a cardinal regulatory system for homeostasis and cancer-related signalling pathways. In this context, the deregulated expression of p62 -Sequestosome1 (p62/SQSTM1)a protein acting both as an autophagy receptor and signalling hub, has been associated with tumour development and chronic inflammation. Multiple clinical studies test drugs targeting autophagy, and even more research is on the way to clinical trials. However, no comparative investigations have been carried out to identify adequate preclinical models to assess p62-based medicine. In veterinary oncology the role of p62 in cancerrelated pathways has been largely ignored. We compared p62 sequences in multiple organisms and found that canine p62 significantly diverges from the humans and from other animals sequences. Then, we chart by immunohistochemistry the expression levels of p62 in canine mammary tumours. A total of 66 tumours and 10 nonneoplastic mammary samples were examined. The expression of p62 was higher in normal tissue and adenomas than carcinomas, with lowest levels of p62 protein detected in high grade carcinomas. In all cases examined the tumour stroma appeared to be p62-negative. Taken together our results would suggest that in dogs the association between p62 expression and cancer cells overturns that reported in human breast carcinoma, where p62 accumulates in malignant cells as compared to normal epithelium. Thus, at least in canine mammary tumours, p62 should be not considered a tumour-rejection antigen for an anti-cancer immunotherapy. K E Y W O R D Sautophagy, dog, gene homology, immunohistochemistry, mammary tumours, p62/SQSTM1

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Safety and efficacy of p62 DNA vaccine ELENAGEN in a first-in-human trial in patients with advanced solid tumors

Cited by 25 publications

References 47 publications

p62/SQSTM1 – steering the cell through health and disease

p62/SQSTM1 – steering the cell through health and disease

Recent clinical trials of cancer immunogene therapy in companion animals

p62/SQSTM1 expression in canine mammary tumours: Evolutionary notes

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