In the last decades, significant progress in research and clinics has been made to offer possible innovative therapeutics for the management of allergic diseases. However, current allergen immunotherapy shows limitations concerning the long-term efficacy and safety due to local side effects and risk of anaphylaxis. Thus, effective and safe vaccines with reduced dose of allergen have been developed using adjuvants. Nevertheless, the use of adjuvants still has several disadvantages, which limits its use in human vaccines. In this context, several novel adjuvants for allergen immunotherapy are currently being investigated and developed. Currently, nanoparticles-based allergen-delivery systems have received much interest as potential adjuvants for allergen immunotherapy. It has been demonstrated that the incorporation of allergens into a delivery system plays an important role in the efficacy of allergy vaccines. Several nanoparticles-based delivery systems have been described, including biodegradable and nondegradable polymeric carriers. Therefore, this paper provides an overview of the current adjuvants used for allergen immunotherapy. Furthermore, nanoparticles-based allergen-delivery systems are focused as a novel and promising strategy for allergy vaccines.
Ivermectin is an FDA-approved broad-spectrum antiparasitic agent with demonstrated antiviral activity against a number of DNA and RNA viruses, including severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Despite this promise, the antiviral activity of ivermectin has not been consistently proven
in vivo
. While ivermectin's activity against SARS-CoV-2 is currently under investigation in patients, insufficient emphasis has been placed on formulation challenges. Here, we discuss challenges surrounding the use of ivermectin in the context of coronavirus disease-19 (COVID-19) and how novel formulations employing micro- and nanotechnologies may address these concerns.
Myocardial infarction is the most significant manifestation of ischemic heart
disease and is associated with high morbidity and mortality. Novel strategies
targeting at regenerating the injured myocardium have been investigated,
including gene therapy, cell therapy, and the use of growth factors. Growth
factor therapy has aroused interest in cardiovascular medicine because of the
regeneration mechanisms induced by these biomolecules, including angiogenesis,
extracellular matrix remodeling, cardiomyocyte proliferation, stem-cell
recruitment, and others. Together, these mechanisms promote myocardial repair
and improvement of the cardiac function. This review aims to address the
strategic role of growth factor therapy in cardiac regeneration, considering its
innovative and multifactorial character in myocardial repair after ischemic
injury. Different issues will be discussed, with emphasis on the regeneration
mechanisms as a potential therapeutic resource mediated by growth factors, and
the challenges to make these proteins therapeutically viable in the field of
cardiology and regenerative medicine.
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