Oral Delivery of Glutamic Acid Decarboxylase (GAD)-65 and IL10 by<i>Lactococcus lactis</i>Reverses Diabetes in Recent-Onset NOD Mice

Robert, Sofie; Gysemans, Conny; Takiishi, Tatiana; Korf, Hannelie; Spagnuolo, Isabella; Sebastiani, Guido; Huynegem, Karolien Van; Steidler, Lothar; Caluwaerts, Silvia; Demetter, Pieter; Wasserfall, Clive; Atkinson, Mark A.; Dotta, Francesco; Rottiers, Pieter; Belle, Tom L. Van; Mathieu, Chantal

doi:10.2337/db13-1236

Cited by 127 publications

(89 citation statements)

References 50 publications

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“…Responding mice showed normal glucose levels in blood, and remained responsive to other antigens, suggesting an antigen-specific immunosuppression. A similar combination therapy based on anti-CD3 Abs and the oral delivery of engineered L. lactis secreting IL-10 and the diabetes-related auto-antigen glutamic acid decarboxylase (GAD)-65 has been reported [17]. This combination was effective in the treatment of advanced stages of T1D with severe hyperglycemia.…”

Section: Engineered Bacteria Against Inflammatory and Autoimmune Disomentioning

confidence: 93%

Engineered bacteria as therapeutic agents

Piñero-Lambea

Ruano-Gallego

Fernández

2015

Current Opinion in Biotechnology

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Although bacteria are generally regarded as the causative agents of infectious diseases, most bacteria inhabiting the human body are non-pathogenic and some of them can be turned, after proper engineering, into 'smart' living therapeutics of defined properties for the treatment of different illnesses. This review focuses on recent developments to engineer bacteria for the treatment of diverse human pathologies, including inflammatory bowel diseases, autoimmune disorders, cancer, metabolic diseases and obesity, as well as to combat bacterial and viral infections. We discuss significant advances provided by synthetic biology to fully reprogram bacteria as human therapeutics, including novel measures for strict biocontainment.

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Section: Engineered Bacteria Against Inflammatory and Autoimmune Disomentioning

confidence: 93%

Engineered bacteria as therapeutic agents

Piñero-Lambea

Ruano-Gallego

Fernández

2015

Current Opinion in Biotechnology

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“…LAB have been also engineered to induce mucosal immune tolerance of causative antigens in food allergies, such coeliac disease (Huibregtse et al ., 2009). Induction of tolerance has also been applied to downregulate autoimmune diseases like type 1 diabetes (T1D), in which self‐antigens from pancreatic β‐cells are recognized by the immune system (Takiishi et al ., 2012; Robert et al ., 2014). In addition, engineered bacteria can modulate levels of cytokines outside the GIT, preventing cardiovascular pathologies (Jing et al ., 2011) and encephalomyelitis (Rezende et al ., 2013).…”

Section: Engineered Bacteria Against Immunological and Metabolic Disementioning

confidence: 99%

Sustainable therapies by engineered bacteria

Álvarez

Fernández

2017

Microbial Biotechnology

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SummaryThe controlled in situ delivery of biologics (e.g. enzymes, cytokines, antibodies) by engineered bacteria of our microbiome will allow the sustainable production of these complex and expensive drugs locally in the human body, overcoming many of the technical and economical barriers currently associated with the global use of these potent medicines. We provide examples showing how engineered bacteria can be effective treatments against multiple pathologies, including autoimmune and inflammatory diseases, metabolic disorders, diabetes, obesity, infectious diseases and cancer, hence contributing to achieve the Global Sustainable Goal 3: ensure healthy lives and promote well‐being for all at all ages.

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“…L. lactis (AG013) has also been modified to secrete trefoil factor 1 for the treatment of oral mucositis, and is currently in Phase Ib clinical trials [50]. Mucosal delivery of recombinant L. lactis MG1363 secreting the diabetic autoantigen proinsulin or glutamic acid decarboxylase (GAD 65) along with IL-10 reversed T1D in NOD (non obese diabetic) mice [51,52], while oral vaccination with recombinant L. plantarum NCL21 expressing a common Japanese cedar pollen allergen, Cry j 1(Cry j 1-LAB), ameliorated the symptoms of cedar pollinosis and decreased allergen-specific IgE production in a murine model of cedar pollinosis [53]. A recent progress made in the application of LAB as live mucosal vectors is the production and delivery of GLP-1 and GLP-1analogs for the treatment of T2DM.…”

Section: Genetically Engineered Food-grade Bacteria As Delivery Systemsmentioning

confidence: 99%