Sustained Interleukin-10 Transgene Expression Following Intra-Articular AAV5-IL-10 Administration to Horses

Moss, Kaitlyn L.; Jiang, Zibin; Dodson, Michael E.; Linardi, Renata L.; Haughan, Joanne; Gale, Alexis L.; Grzybowski, Cara; Engiles, Julie E.; Stefanovski, Darko; Robinson, Mary Ann; Ortved, Kyla F.

doi:10.1089/hum.2019.195

Cited by 24 publications

(39 citation statements)

References 30 publications

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“…Some of the experimental procedures described below can be found in more detail in a published paper by Moss et al 21 …”

Section: Methodsmentioning

confidence: 99%

“…A rAAV‐IL10 viral vector was generated by the University of North Carolina Vector Core as described previously 21 . Briefly, the vector consisted of an equine IL‐10 transgene, flanked by AAV2 inverted terminal repeats (ITRs) and under control of a cytomegalovirus (CMV) promoter (Figure 1) incorporated into the AAV5 viral capsule.…”

Section: Methodsmentioning

confidence: 99%

“…There are many serotypes of AAV and appropriate rAAV vectors are chosen for specific applications based on tissue tropism and transduction efficiency 13–16 . In horses, rAAVs have predominantly been used for intra‐articular delivery of anti‐inflammatory or anabolic genes such as IL1‐RA, 14,15,17,18 IGF‐1, 19,20 and most recently, IL‐10 21 …”

Section: Introductionmentioning

confidence: 99%

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Detection of intra‐articular gene therapy in horses using quantitative real time PCR in synovial fluid and plasma

Haughan

Jiang

Stefanovski

et al. 2020

Drug Testing and Analysis

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Gene therapy promotes the expression of missing or defective genes and can be curative following administration of a single dose. Gene therapy is prohibited in equine athletes by regulatory bodies due to the high potential for abuse and novel analytical methods are needed for detection. The goal of this study was to detect the administration of an experimental gene therapy: a recombinant adeno‐associated viral vector (rAAV) carrying a transgene for the anti‐inflammatory cytokine IL‐10 (rAAV‐IL10). Twelve horses were randomly assigned to receive an intra‐articular injection of rAAV‐IL10 or phosphate buffered saline (vehicle) into a middle carpal joint. Plasma and synovial fluid were collected on days 0, 1, 2, 4, 7, 14, 28, 56, and 84. Primer pairs were designed to detect two unique regions of rAAV. Using quantitative real time PCR, both sets of primers detected rAAV for 14–28 days in joints and up to 4 days in plasma, in all six treated horses. In synovial fluid, rAAV was detected on day 56 in 4/6 horses by both primer sets, and on day 84 in 1/6 horses by one primer set. In plasma, rAAV was detected for 7 days in 5/6 horses, 14 days in 2/6 horses, and 28 days in 1/6 horses by one primer set, and was detected for up to 14 days in 1/6 horses by the other primer set. This study is the first to validate that quantitative real time PCR can be used to systemically detect the local administration of a gene therapy product to horses.

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“…Some of the experimental procedures described below can be found in more detail in a published paper by Moss et al 21 …”

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Detection of intra‐articular gene therapy in horses using quantitative real time PCR in synovial fluid and plasma

Haughan

Jiang

Stefanovski

et al. 2020

Drug Testing and Analysis

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“…Inhibiting IL-17 signaling in the horse will not be as simple as applying human therapies since the most successful psoriasis treatments use monoclonal antibodies to block IL- 17 receptor activation [21]; these antibodies may not bind the equine IL-17 receptor, may be antigenic in equines, and are likely cost-prohibitive. Local inhibition of IL-17 and/or mTORC1 would be desirable, and could be possible using an adeno-associated viral vector to deliver genes for inhibitory cytokines to reduce inflammation, as demonstrated recently [83], or other genes able to inhibit IL-17 and/or mTORC1 activation.…”

Section: Discussionmentioning

confidence: 99%

Interleukin-17 pathway activation inEquus caballussupporting limb laminitis

Cassimeris

Galantino‐Homer

2020

Preprint

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22 Supporting Limb Laminitis (SLL) is a painful and crippling secondary complication of 23 orthopedic injuries and infections in horses, often resulting in euthanasia. Due to altered weight 24 bearing, SLL causes structural alternations and inflammation of the interdigitating layers of 25 specialized epidermal and dermal tissues, the lamellae, which suspend the equine distal phalanx 26 from the hoof capsule. Activation of the interleukin-17 (IL-17)-dependent inflammatory pathway 27 is an epidermal stress response that contributes to physiologic cutaneous wound healing as well 28 as pathological skin conditions. To test the hypothesis that IL-17 pathway activation is involved 29 in equine epidermal lamellae in SLL, we analyzed the expression of the IL-17 receptor subunit A 30 and 11 genes upregulated by IL-17 in lamellar tissue isolated from Thoroughbreds euthanized 31 due to naturally occurring SLL and in age and breed matched non-laminitic controls. The IL-17 32 Receptor A subunit was expressed in both non-laminitic and laminitic tissues. In severe acute 33 SLL (n=7) compared to non-laminitic controls (n=8), quantitative PCR demonstrated ~20-100 34 fold upregulation of ß defensin 4 (E. caballus gene DEFB4B) and S100A9 genes. DEFB4B was 35 also upregulated in developmental (n=8), moderate acute (n=7), and severe chronic (n=5) 36 samples. By RT-PCR, S100A8, MMP9, and PTSG2 (COX2) expression was upregulated in most 37 or all severe acute SLL samples, whereas several other genes, CCL2, CxCL8, TNF, IL6 and 38 MMP1 were detected in some, but not all, severe acute samples. PTGS2, CCL2, TNF and IL6 39 were also expressed in some, but not all, developmental and moderate acute disease stages.40 Moreover, expression of DEFB4 by in situ hybridization and calprotectin (S100A9/S100A8) 41 protein by immunofluorescence was detected in keratinocytes, primarily in suprabasal cell 42 layers, from SLL samples. These data support the hypothesis that the IL-17 inflammatory 3 43 pathway is active in equine SLL, and that similarities exist between equine and human epidermal 44 tissue responses to stresses and/or damage. 4 45 Introduction 46 47 Equine laminitis is a common, progressive, crippling and currently incurable disease 48 often necessitating euthanasia to end suffering from the painful loss of limb support. Healthy 49 lamellar tissue connects the inner hoof wall to the distal phalanx (DP), forming a major 50 component of the suspensory apparatus of the DP, a unique adaptation of equids that allows for 51 suspension of almost the entire weight of the animal through the hoof capsule [1; 2]. The hoof is 52 a modified epidermal appendage integrated into the musculoskeletal system by the epidermal and 53 dermal lamellae, homologous to the nail bed, which are extensively folded to form primary and 54 secondary lamellae to increase the surface area of attachment (Fig 1; [3,4]). Similar to skin, 55 keratin 14 is expressed within lamellar epidermal basal cells [5-7]; however equine epidermal 56 lamellae have several architectural and ...

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“…Recent advances in veterinary medical technologies have enabled gene therapy in horses, and several clinical studies have been reported [4][5][6]. Gene therapy may be technically categorized into gene transfer, gene silencing and gene editing.…”

Section: Introductionmentioning

confidence: 99%

Microfluidic Quantitative PCR Detection of 12 Transgenes from Horse Plasma for Gene Doping Control

Tozaki

Ohnuma

Kikuchi

et al. 2020

Genes

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Gene doping, an activity which abuses and misuses gene therapy, is a major concern in sports and horseracing industries. Effective methods capable of detecting and monitoring gene doping are urgently needed. Although several PCR-based methods that detect transgenes have been developed, many of them focus only on a single transgene. However, numerous genes associated with athletic ability may be potential gene-doping material. Here, we developed a detection method that targets multiple transgenes. We targeted 12 genes that may be associated with athletic performance and designed two TaqMan probe/primer sets for each one. A panel of 24 assays was prepared and detected via a microfluidic quantitative PCR (MFQPCR) system using integrated fluidic circuits (IFCs). The limit of detection of the panel was 6.25 copy/µL. Amplification-specificity was validated using several concentrations of reference materials and animal genomic DNA, leading to specific detection. In addition, target-specific detection was successfully achieved in a horse administered 20 mg of the EPO transgene via MFQPCR. Therefore, MFQPCR may be considered a suitable method for multiple-target detection in gene-doping control. To our knowledge, this is the first application of microfluidic qPCR (MFQPCR) for gene-doping control in horseracing.

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Sustained Interleukin-10 Transgene Expression Following Intra-Articular AAV5-IL-10 Administration to Horses

Cited by 24 publications

References 30 publications

Detection of intra‐articular gene therapy in horses using quantitative real time PCR in synovial fluid and plasma

Detection of intra‐articular gene therapy in horses using quantitative real time PCR in synovial fluid and plasma

Interleukin-17 pathway activation inEquus caballussupporting limb laminitis

Microfluidic Quantitative PCR Detection of 12 Transgenes from Horse Plasma for Gene Doping Control

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