This study provides a review of Molecular Pathways and the Future
Therapeutic Implications for Atopic Dermatitis. No available treatments can
provide long-term remission for patients with moderate to severe Atopic
Dermatitis (AD) creating a large unmet need for effective systemic treatment.
Together with asthma and allergic rhinitis, it constitutes the “Atopic Triad”.
The important factors and related mechanisms for AD are the following: (a)
Genetic, (b) Neurohumoral, (c) Skin barrier dysfunction, and (d) Immunological
mechanisms. Much progress has been made in the understanding of its genetic
background and pathophysiology through studies in genetics, epidemiology, and
immunology. The cellular interactions, molecular events, and pathways for the
pathogenesis of AD were integrated into a hypothesis and reported recently. As
the new insights into the immune and molecular pathways of AD increase, a
variety of experimental agents, particularly biological agents that target
pathogenic molecules bring promise of safe and effective therapeutics. Some of
the most promising biological therapies that are in development or in clinical
trials are based on principles as the following: Barrier repair,
Allergen-specific immunotherapy, Targeted Immunomodulating Therapies (TIT)
(Anti-IgE therapy, Anti-CD20, Inhibition of T-cell responses, Th2-cell
inhibition strategies/ Anti IL-4 therapies, Anti IL-5 strategies, Anti IL-31),
Targeting Th22, Targeting Th17/IL-12/IL-23 pathway, Recombinant IFN-y, Anti
IL-6R, Anti TNF agents, Phosphodiesterase inhibitors, PPAR-gamma agonists.
All these biological therapies are at different phases of clinical
trials. There has been a growing trend toward the use of targeted therapies in
treating AD in recent years. These
biological agents would potentially hold great promise for the treatment of AD
if they can offer advantages, i.e. low toxicity, good efficacy, improved
patient compliance via weekly/biweekly/and even monthly administration,
reduction of disease activity, relapse prevention, etc. In Summary, the recent
advances in understanding the immunopathogenic mechanisms provide an opportunity
for the development of biological therapies directed at pathways driving AD.
This is possibly the beginning of an exciting era in AD therapeutics with the
impending availability of drugs having low toxicity and increased patient
compliance. These expected drugs will not only treat this disease but also
prevent the development and relapse of new skin lesions. In this article,
attempts have been made to provide an updated account of these new
possibilities. The recent advances in our understanding of the immunopathogenic
mechanisms implicated in AD provide an opportunity for the development of
biological therapies directed at pathways driving AD.
Author
(s) Details
ASM Giasuddin
Medical Research Unit (MRU), MHWT, Plot-4 Road-9 Sector-1, Uttara Model Town,
Dhaka-1230, Bangladesh.
Shafiqul Islam
Department of Dermatology, Medical College for Women & Hospital
(MCW&H), MRU, MHWT Plot-4 Road-9 Sector-1, Uttara Model Town, Dhaka-1230,
Bangladesh.
Khadija Akther Jhuma
Department of Biochemistry, MCW&H, Member Secretary, MRU, MHWT Plot-4
Road-9 Sector-1, Uttara Model Town, Dhaka-1230, Bangladesh.
AM Mujibul Haq
Department of Medicine, MCW&H & Chairman Projects and Chairman,
MRU, MHWT, Plot-4 Road-9 Sector-1, Uttara Model Town, Dhaka-1230, Bangladesh.
Please see the book here:- https://doi.org/10.9734/bpi/crpbs/v3/2459
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