A Coxsackievirus B vaccine protects against virus-induced diabetes in an experimental mouse model of type 1 diabetes

Stone, Virginia M.; Hankaniemi, Minna M.; Svedin, Emma; Sioofy‐Khojine, Amir‐Babak; Oikarinen, Sami; Hyöty, Heikki; Laitinen, Olli H.; Hytönen, Vesa P.; Flodström‐Tullberg, Malin

doi:10.1007/s00125-017-4492-z

Cited by 51 publications

(65 citation statements)

References 11 publications

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“…Effective and safe vaccines have been developed against polioviruses and enterovirus 71, but there are no vaccines available for the enteroviruses linked to type 1 diabetes. Recent preclinical studies provided proof-of-concept that a CVB vaccine prevents viral infection and diabetes induction in mice harbouring beta cells genetically permissive to CVB infection [ 52 ]. It is critical to determine which virus serotypes are associated with type 1 diabetes in different geographical regions over various periods.…”

Section: Rationale For the Development Of A Vaccinementioning

confidence: 99%

Rationale for enteroviral vaccination and antiviral therapies in human type 1 diabetes

et al. 2019

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In type 1 diabetes, pancreatic beta cells are destroyed by chronic autoimmune responses. The disease develops in genetically susceptible individuals, but a role for environmental factors has been postulated. Viral infections have long been considered as candidates for environmental triggers but, given the lack of evidence for an acute, widespread, cytopathic effect in the pancreas in type 1 diabetes or for a closely related temporal association of diabetes onset with such infections, a role for viruses in type 1 diabetes remains unproven. Moreover, viruses have rarely been isolated from the pancreas of individuals with type 1 diabetes, mainly (but not solely) due to the inaccessibility of the organ. Here, we review past and recent literature to evaluate the proposals that chronic, recurrent and, possibly, persistent enteroviral infections occur in pancreatic beta cells in type 1 diabetes. We also explore whether these infections may be sustained by different virus strains over time and whether multiple viral hits can occur during the natural history of type 1 diabetes. We emphasise that only a minority of beta cells appear to be infected at any given time and that enteroviruses may become replication defective, which could explain why they have been isolated from the pancreas only rarely. We argue that enteroviral infection of beta cells largely depends on the host innate and adaptive immune responses, including innate responses mounted by beta cells. Thus, we propose that viruses could play a role in type 1 diabetes on multiple levels, including in the triggering and chronic stimulation of autoimmunity and in the generation of inflammation and the promotion of beta cell dysfunction and stress, each of which might then contribute to autoimmunity, as part of a vicious circle. We conclude that studies into the effects of vaccinations and/or antiviral drugs (some of which are currently on-going) is the only means by which the role of viruses in type 1 diabetes can be finally proven or disproven.

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Section: Rationale For the Development Of A Vaccinementioning

confidence: 99%

Rationale for enteroviral vaccination and antiviral therapies in human type 1 diabetes

et al. 2019

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“…Recently, further collaboration studies were set out to test whether the inactivated CVB vaccine preventing CVB infection could also prevent virusinduced diabetes in mice. These studies first confirmed that CVB infection can accelerate diabetes onset in NOD and SOCS-1-Tg mice and then proved that the CVB vaccine protects not only from CVB infection but also against CVB-induced diabetes development in SOCS-1-Tg mice [110].…”

Section: Preclinical Development Of a Cvb Vaccine Against T1dmentioning

confidence: 69%

Developing a vaccine for type 1 diabetes by targeting coxsackievirus B

Hyöty

León²,

Knip

2018

Expert Review of Vaccines

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Introduction: Virus infections have long been considered as a possible cause of type 1 diabetes (T1D). One virus group, enteroviruses (EVs), has been studied extensively, and clinical development of a vaccine against T1D-associated EV types has started. Areas covered: Epidemiological studies have indicated an association between EVs and T1D. These viruses have a strong tropism for insulin-producing β-cells; the destruction of these cells leads to T1D. The exact mechanisms by which EVs could cause T1D are not known, but direct infection of β-cells and virus-induced inflammation may play a role. Recent studies have narrowed down the epidemiological association to a subset of EVs: group B coxsackieviruses (CVBs). These findings have prompted efforts to develop vaccines against CVBs. Prototype CVB vaccines have prevented both infection and CVB-induced diabetes in mice. This review summarizes recent progress in the field and the specifics of what could constitute the first human vaccine developed for a chronic autoimmune disease. Expert commentary: Manufacturing of a clinical CVB vaccine as well as preclinical studies are currently in progress in order to enable clinical testing of the first CVB vaccine. Ongoing scientific research projects can significantly facilitate this effort by providing insights into the mechanisms of the CVB-T1D association.

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“…In a followup study, the vaccine was tested on suppressor of cytokine signaling transgenic (SOCS1-tg) mice, in which beta cells are unable to respond to IFNs and have an increased susceptibility to EV infection [80]. Similarly to NOD mice, SOCS1-tg mice developed a robust antibody response, were protected from a CVB1 challenge and from diabetes and had normal pancreas morphology [80]. The studies exposed above and the identification of different EVs serotypes with possible roles in T1D suggest that the development of an EVs vaccine for T1D could have great benefits, but could be challenging to produce.…”

Section: Calling For Reinforcements Co-operation Is the Keymentioning

confidence: 99%

Enterovirus infection and type 1 diabetes: unraveling the crime scene

Rodríguez-Calvo

2018

Clinical and Experimental Immunology

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Summary Enteroviruses (EV) have been historically associated to type 1 diabetes. Definitive proof for their implication in disease development is lacking, but growing evidence suggests that they could be involved in beta cell destruction either directly by killing beta cells or indirectly by creating an exacerbated inflammatory response in the islets, capable of attracting autoreactive T cells to the ‘scene of the crime’. Epidemiological and serological studies have been associated with the appearance of islet autoimmunity and EV RNA has been detected in prospective studies. In addition, the EV capsid protein has been detected in the islets of recent‐onset type 1 diabetic donors, suggesting the existence of a low‐grade EV infection that could become persistent. Increasing evidence in the field shows that a ‘viral signature’ exists in type 1 diabetes and involves interferon responses that could be sustained during prolonged periods. These include the up‐regulation of markers such as protein kinase R (PKR), melanoma differentiation‐associated protein 5 (MDA5), retinoic acid inducible gene I (RIG‐I), myxovirus resistance protein (MxA) and human leukocyte antigen‐I (HLA‐I) and the release of chemokines able to attract immune cells to the islets leading to insulitis. In this scenario, the hyperexpression of HLA‐I molecules would promote antigen presentation to autoreactive T cells, favoring beta cell recognition and, ultimately, destruction. In this review, an overview is provided of the standing evidence that implicates EVs in beta cell ‘murder’, the time‐line of events is investigated from EV entry in the cell to beta cell death and possible accomplices are highlighted that might be involved in beta cell demise.

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A Coxsackievirus B vaccine protects against virus-induced diabetes in an experimental mouse model of type 1 diabetes

Cited by 51 publications

References 11 publications

Rationale for enteroviral vaccination and antiviral therapies in human type 1 diabetes

Rationale for enteroviral vaccination and antiviral therapies in human type 1 diabetes

Developing a vaccine for type 1 diabetes by targeting coxsackievirus B

Enterovirus infection and type 1 diabetes: unraveling the crime scene

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