Androgenetic Alopecia Clinical Trial
Official title:
Topical Cetirizine Gel Versus Minoxidil 5% Gel in Treatment of Androgenetic Alopecia
Androgenetic alopecia (AGA), also known as androgenic alopecia or male pattern baldness, is
the most common type of progressive hair loss. It is a polygenetic condition with variable
degree of severity, age of onset, and location of hair loss.
Male AGA (MAGA) is clearly an androgen-dependent condition and, although the mode of
inheritance is uncertain, a genetic predisposition is observed.
Regarding treatment of AGA; in most cases it's challenging and unsatisfactory. Finasteride
and Minoxidil 2-5 % solution are the only US Food and Drug Administration (FDA) approved
treatment options for MAGA.
On the basis of hypertrichosis observed in patients treated with analogues of prostaglandin
PGF2a (i.e. latanoprost used for glaucoma), it was supposed that prostaglandins would have an
important role in the hair growth (Nieves et al., 2014).
Multiple studies had claimed that prostaglandins are deregulated in both alopecia areata (AA)
and AGA.
Cetirizine, is a safe and selective second-generation histamine H1 receptor antagonist widely
used. It has anti-inflammatory properties. Studies have shown cetirizine causes a significant
reduction in both the inflammatory cell infiltrate and PGD2 production.
The oral administration of cetirizine is commonly leads to different systemic side effects.
Thus the topical formulation is expected to be an effective tool for avoiding the oral side
effects as well as better targeting, but unfortunately, no topical formulation of cetirizine
is available in the market till date.
Androgenetic alopecia (AGA), also known as androgenic alopecia or male pattern baldness, is
the most common type of progressive hair loss. It is a polygenetic condition with variable
degree of severity, age of onset, and location of hair loss.
Hair loss typically begins with bi-temporal recession of the frontal hairline, followed by
diffuse hair thinning at the vertex, and eventual complete loss of hair at the center of the
vertex. The bald patch at the vertex subsequently joins the frontal receding hairline,
leaving an island of hair on the frontal scalp, which finally disappears leaving hair only in
the parietal and occipital zones producing the characteristic "horseshoe" pattern.
Androgenetic alopecia is classified according to the Hamilton-Norwood scale into grades (from
I to VII).
AGA features a progressive miniaturization of the hair follicle leading to vellus
transformation of terminal hair which results from an alteration in hair cycle dynamics:
anagen phase duration gradually decreases and that of the telogen phase increases. As the
anagen phase duration determines hair length, the new anagen hair becomes shorter, eventually
leading to bald appearance.
The etiology of AGA is multifactorial and polygenetic. Male AGA (MAGA) is clearly an
androgen-dependent condition and, although the mode of inheritance is uncertain, a genetic
predisposition is observed, while in female AGA (FAGA) the role of androgens is still
uncertain.
Regarding treatment of AGA; in most cases it's challenging and unsatisfactory. Finasteride
and Minoxidil 2-5 % solution are the only US Food and Drug Administration (FDA) approved
treatment options for MAGA.
Finasteride is a type 2 5α-reductase inhibitor that decreases the conversion of testosterone
to dihydrotestosterone (DHT), which is responsible for the miniaturization of the hair
follicle seen in MAGA.
Minoxidil is a direct arteriolar vasodilator acts by opening potassium channels. Unwanted
hair growth was observed as an adverse effect in 24-100 % of patients treated by Minoxidil
for hypertension. Minoxidil 2 % solution was approved in 1988, while the 5 % solution was
approved in 1991, and the 5 % foam in 2016 for MAGA.
On the basis of hypertrichosis observed in patients treated with analogues of prostaglandin
PGF2a (i.e. latanoprost used for glaucoma), it was supposed that prostaglandins would have an
important role in the hair growth.
Their action is variable depending on the class they belong to: PGE and PGF2a play a
generally positive role on the hair growth, while PGD2 an inhibitory role on the hair growth.
Multiple studies had claimed that prostaglandins are deregulated in both alopecia areata (AA)
and AGA.
Garza in 2012 found elevated levels of prostaglandin D2 synthase (PTGDS) at the mRNA and
protein levels in bald scalp versus haired scalp of men with AGA. Also found that the
enzymatic product of PTGDS and prostaglandin D2 (PGD2) are raised in bald human scalp tissue.
These results implicate that PGD2 might has a role in pathogenesis of AGA, thus suggest new
receptor targets for its treatment.
Cetirizine, the active carboxylic acid metabolite of hydroxyzine, is a safe and selective
second-generation histamine H1 receptor antagonist widely used in daily practice. It has
anti-inflammatory properties and high specific affinity for histamine H1 receptors. Studies
have shown cetirizine causes a significant reduction in both the inflammatory cell infiltrate
and PGD2 production, and these effects are not related to its anti-H1 activity.
The oral administration of cetirizine is commonly leads to different systemic side effects as
sedation, ocular dryness, tiredness and dry mouth. Thus, the topical formulation for
cetirizine is expected to be a rational and effective tool for avoiding the oral side effects
as well as better targeting, but unfortunately, no topical formulation of cetirizine is
available in the market till date.
As the stratum corneum is the main barrier for the effective topical drug application,
numerous attempts have been made to enhance topical drug delivery such as lipid nanocarriers
(nano-transferosomes (NTF), follicular penetration, microbubbles and microneedles.
Rossi in 2018 evaluated for the first time in literature the tolerability and efficacy of
topical cetirizine 1% lotion inpatients with AGA and claimed that topical cetirizine causes a
significant improvement of the initial framework of AGA in both males and females and
recommended further studies to allow better investigation for the role of cetirizine in AGA.
To the best of the investigators knowledge the use of topical cetirizine 1% gel has not yet
been tried in the therapeutic management of Egyptian males with AGA.
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