The flavonoid hesperidin exerts anti-photoaging effect by downregulating matrix metalloproteinase (MMP)-9 expression via mitogen activated protein kinase (MAPK)-dependent signaling pathways

Aging is a process of progressive reduction in the maximal function and reserve capacity of all body organs including the skin [1]. Skin aging can be classified into two types, intrinsic aging (chronological) and extrinsic aging (photoaging) [2]. Intrinsic aging is a biological process common to all living organisms, and is characterized by an age-dependent deterioration of the skin function and structure, such as epidermal atrophy and dermal-epidermal junctional flattening [3]. In contrast, extrinsic aging (photoaging) results from chronic exposure of the skin to sunlight, and is characterized by histological changes, including damage to collagen fibers and excessive deposition of abnormal elastic fibers [4] UV irradiation induces changes in the physiologic and biochemical features of the skin that lead to increase in the epidermal thickness, skin damage and skin dehydration, and transepidermal water loss (TEWL) [5].

UV irradiation-activated receptors lead to intracellular signaling through stimulation of the stress-associated mitogen-activated protein kinases (MAPK) that regulate the expression of matrix metalloproteinase (MMP)-9 and induce transcriptional factors [6]. UV-irradiated photodamaged skin shows reduced collagen synthesis, and increased levels and activity of MMPs, specifically MMP-1, MMP-3, and MMP-9 [7]. Degradation of extracellular matrix components by MMPs is an important event in common biological processes [8]. For example, MMPs are involved in the extracellular matrix remodeling and play important roles in morphogenesis, angiogenesis, skin ulceration, tumor invasion, and photoaging [9]. MMPs are suggested to be UV-induced aging factors [10]. Even extremely low levels of UVB irradiation can upregulate the MMP activity in human skin. In addition, UV irradiation activates the nuclear factor-kappa B (NF-κB) transcription factor that induces the expression of pro-inflammatory cytokines, proteins involved in immunoregulation, and stimulates the expression of MMPs [11]. UVB-induced inflammatory response is characterized by acute development of edema and erythema, increase in dermal inflammatory cell infiltrates, and augmented prostaglandin synthesis [12]. Moreover, there is an increase in pro-inflammatory cytokines, such as tumor necrosis factor alpha (TNF-α), interleukin (IL)-1β, and IL-8, that accelerates the skin damage and results in MMP activation [13]. In this study, we used hairless mice model for studying photoaging that suitable for studying histological changes of photoaged skin such as wrinkle formation as induced by UVB irradiation [14, 15]. Therefore, the present study examined the effects of the oral administration of hesperidin on UVB-induced hairless mice model including wrinkle formation, MMP-9 expression, and anti-inflammatory effects.

Hesperidin [3′,5,7-trihydroxy-4′-methoxyflavanone-7-(6-α-l-rhamnopyranosyl-β-d-glucopyranoside)], a flavanone glycoside comprising an aglycone hesperetin and an attached disaccharide rutinose, is found abundantly in citrus fruits and has been reported to exert a wide range of pharmacological effects [16, 17] (Fig. 1). For example, hesperidin exhibited pronounced anticancer activity against some selected human carcinoma cell lines and showed anti-inflammatory effects [18]. However, little is known about the effect of hesperidin on UVB-induced skin cell or animal model. So, in previous study, hesperidin shielded human keratinocytes from UVB radiation-induced damage and apoptosis via its antioxidant and UVB absorption properties [19]. Also, in many previous studies, the orally administrated compounds are absorbed into the body, so they have a photoprotective effects on UVB-induced animal models [20, 21]. In this study, we used male HR-1 hairless mice to assess the protective effect of hesperidin on photoaging. We examined the effect of hesperidin on UVB-induced photoaging in the skin of hairless mice by evaluating various parameters of photoaging.

It is well known that UV radiations from sunlight are a major environmental factor that cause acute and chronic changes in the human skin [22]. Chronic exposure to UV radiation is known to be a primary cause of skin photoaging, which is characterized by skin wrinkles, roughness, laxity, irregular pigmentation, telangiectasia, atrophy, and neoplasia [23].

Hesperidin is a flavanone glycoside abundantly found in sweet orange and lemon [17]. It has a wide range of biological effects, including attenuation of UVB-induced apoptosis mediated by mitigation of oxidative stress in human keratinocytes [24]. Furthermore, it has been reported that phytochemicals such as proanthocyanidin, genistein, and daidzein are potential photoprotective agents against UVB-induced skin damage [25, 26]. Previous studies have shown that flavonoids can be used orally to protect the skin from UVB-induced damage [27, 28]. For example, quercetin inhibited the UV irradiation-induced inflammatory cytokine production in primary human keratinocytes by suppressing the NF-κB pathway [29]. Furthermore in this study, we demonstrated that the natural flavonoid hesperidin exerts anti-photoaging effect by activating MMP-9 expression via the MAPK signaling pathways on UVB-induced hairless mice model. In this study, we investigated the anti-photoaging effects of hesperidin against UVB-irradiation on the dorsal skin of HR-1 mice. Histological studies have shown that photoaging of the skin is associated with increased epidermal thickness and alterations in the connective tissue organization [30]. Similarly, we found that chronic UVB irradiation of the mice dorsal skin induced wrinkle formation and epidermal thickening. Hesperidin improved these damages induced by UVB.

Epidermal thickness is used as a quantitative parameter for assessing inflammation and skin photoaging [31]. UVB irradiation causes skin damage, leading to skin dehydration and an increase in TEWL [32]. Increased TEWL impairs enzymatic functions that result in the visible appearance of dry and aged skin [33]. Because UV irradiation of the skin disrupts the epidermal permeability barrier function, TEWL is an important parameter to be assessed in the studies of skin photoprotective effects [34]. Hesperidin treatment effectively reduced skin damage in this study. This was associated with an increase in skin hydration and decreases in TEWL.

MMPs are zinc-dependent endopeptidases associated with extracellular matrix remodeling that play important roles in morphogenesis, angiogenesis, arthritis, skin ulceration, tumor invasion, and photoaging [35]. MMP expression induced by UVB exposure leads to the degradation of the extracellular matrix, including collagen fibers, and thus contributes to skin wrinkle formation [36]. UVB irradiation is specifically associated to the expression of MMP-1, −3, and −9 in the normal human epidermis in vivo, which indicates that MMPs are the main UVB-induced aging factors [10, 37]. UV irradiation of the skin leads to MMP-9 formation, which degrades collagen type IV, an important component of the basement membrane in the skin dermal epidermal junction [38, 39]. Hesperidin ameliorated the photoaging in the dorsal skin of mice by downregulating the expression and activity of MMP-9.

UVB-induced cytokines act in a cascade to induce inflammation. They are initially released by keratinocytes or inflammatory cells in the skin after UVB irradiation, and subsequently synergize with UV-irradiated keratinocytes to further increase their production [40]. TNF-α, and IL-8 are important regulators of the intensity of inflammatory reactions that occur during the host response to injurious stimuli such as UVB radiations that cause severe sunburn reaction [41]. MAPKs are known to regulate the expression of MMP-9, it showed that the inhibition of MMP-9 expression in human dermal fibroblasts was mediated by inhibition of the MEK/ERK signaling pathway [6]. It has been reported that the activation of MEK/ERK signaling is responsible for the induction of MMP-9 and is required for responses in epidermal keratinocytes [42]. Therefore, the UVB-induced phosphorylation of MEK/ERK may be an important molecular target for controlling the MMP expression by anti-photoaging treatments. Results of this study showed that hesperidin attenuated the UVB-induced MMP-9 expression regulated by the MEK/ERK pathway.

In summary, our results showed that hesperidin inhibited the MMP-9 related signaling pathway activated by UVB irradiation. Furthermore, hesperidin prevented the UVB-induced skin thickening, wrinkle formation, and inflammation. Elucidation of the detailed mechanism of MMP-9 inhibition requires further investigation. It can be suggested that hesperidin could be a good candidate as a photoprotective agent for skin care.