KR20190133978A - Pharmaceutical composition for preventing or treating of macular degeneration comprising Prunella vulgaris var. lilacina extract as an active ingredient - Google Patents
Pharmaceutical composition for preventing or treating of macular degeneration comprising Prunella vulgaris var. lilacina extract as an active ingredient Download PDFInfo
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- KR20190133978A KR20190133978A KR1020180059061A KR20180059061A KR20190133978A KR 20190133978 A KR20190133978 A KR 20190133978A KR 1020180059061 A KR1020180059061 A KR 1020180059061A KR 20180059061 A KR20180059061 A KR 20180059061A KR 20190133978 A KR20190133978 A KR 20190133978A
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Abstract
Description
본 발명은 하고초 추출물을 유효성분으로 함유하는 황반변성 예방, 치료 또는 개선용 조성물에 관한 것이다.The present invention relates to a composition for the prevention, treatment or improvement of macular degeneration containing an extract of Hagocho as an active ingredient.
황반은 망막의 중심부에 위치한 신경조직으로 시세포가 밀집되어 있으며, 물체의 상이 맺히는 곳으로 중심시력을 담당한다. 황반은 노화, 유전적 요인, 독성 및 염증 등 여러 가지 원인에 의해 변성이 일어나 시력장애를 일으킬 수 있는데, 이를 황반변성이라고 한다. 황반변성은 녹내장, 당뇨망막증과 함께 실명의 3대 원인 중의 하나이며, 황반에 변성이 생기면 시력감소, 중심암점, 변시증(사물이 찌그러져 보이는 증상) 등이 나타난다.The macula is a neural tissue located in the center of the retina, where the cells of the eye are concentrated, and the central image is the place where the image of the object is formed. Macular degeneration may occur due to various causes such as aging, genetic factors, toxicity and inflammation, which may cause visual disturbances. Macular degeneration is one of the three major causes of blindness along with glaucoma and diabetic retinopathy. Degeneration of the macula leads to decreased vision, central dark spots, and opacity.
황반변성은 건성(비삼출성) 황반변성과 습성(삼출성) 황반변성으로 나뉠 수 있으며, 황반변성의 약 90%는 건성 황반변성에 해당한다. 건성 황반변성은 망막색소상피(retinal pigment epithelium)에 드루젠(drusen)이라는 노폐물이 쌓여 황반부 조직이 얇아지거나 위축된 상태를 말한다. 한편, 습성 황반변성은 황반부에 비정상적으로 성장한 신생혈관이 파열되어 황반으로 혈액이나 점액이 누수된 결과 심각한 시력 상실을 일으키는 것을 말한다. 건성 황반변성은 초기에는 자각증상이 없고 병이 진행되어 증상이 나타난다 하더라도 단순한 노안으로 착각되어 방치하기 쉽다. 하지만, 건성 황반변성이 계속 방치되면 심각한 시력상실이 올 수 있고, 실명율이 높은 습성 황반변성으로 전환되는 경우도 있으므로 건성 황반변성을 예방하는 것이 중요하다.Macular degeneration can be divided into dry (non-exudative) macular degeneration and wet (exudative) macular degeneration. About 90% of macular degeneration is equivalent to dry macular degeneration. Dry macular degeneration is a condition in which macular tissues become thin or atrophy due to the accumulation of drusen waste in the retinal pigment epithelium. On the other hand, wet macular degeneration is an abnormal growth of new blood vessels in the macula rupture blood and mucus leaking into the macula causes severe vision loss. Dry macular degeneration is not subjective at first, and even if the disease progresses, symptoms may be mistaken for simple presbyopia. However, if dry macular degeneration is left unattended, severe macular degeneration may occur, and it is important to prevent dry macular degeneration because it may be converted into wet macular degeneration with high blindness.
황반변성의 근원적인 메커니즘은 아직까지 알려져 있지 않으나, 다인성 병인기전이 영향을 끼치며, 망막색소상피의 변형이 주요 발생인자일 것으로 예측된다. 눈의 노화에 의해 망막색소상피의 리소좀에는 리포푸신(lipofuscin)이 축적되는데, 이는 지질과 단백질의 혼합물뿐 아니라 A2E(N-retinyl-N-retinylidene ethanolamine)라고 부르는 형광색소로 구성되어 있다. A2E는 망막색소상피세포를 사멸시키는 주요 인자로 리소좀에 축적되어 그 기능을 저해함으로써 망막색소상피세포를 사멸시킨다. 특히 A2E는 자외선이나 청색광을 조사하면 반응성이 높은 광산화된 형태로 변하여 미토콘드리아의 단백질 활성을 변화시킴으로써 세포사멸을 유도한다. 또한, A2E에 의한 망막색소상피세포의 사멸은 망막색소상피세포로부터 주요 물질을 공급받는 광수용체(photoreceptor)세포의 2차적 사멸로 이어지며, 특히 황반은 광수용체세포가 밀집되어 있는 곳이기 때문에 그 손상이 가장 크게 나타나 황반변성을 유발한다.The underlying mechanism of macular degeneration is not yet known, but multifactorial etiology affects, and retinal pigment epithelial deformity is expected to be a major factor. As the eyes age, liposomes accumulate in the lysosomes of the retinal pigment epithelium, consisting of a mixture of lipids and proteins, as well as a fluorescent pigment called A2E ( N- retinyl - N - retinylidene ethanolamine). A2E is a major factor that kills retinal pigment epithelial cells and accumulates in lysosomes and inhibits their function, thereby killing retinal pigment epithelial cells. In particular, when A2E is irradiated with ultraviolet light or blue light, it becomes a highly reactive photooxidized form and induces apoptosis by changing the protein activity of mitochondria. In addition, A2E killing of retinal pigment epithelial cells leads to secondary killing of photoreceptor cells, which are supplied with major substances from retinal pigment epithelial cells. The most damaging is the cause of macular degeneration.
한편, 하고초(Prunella Spike)는 꿀풀과(Labiatae)에 속하는 다년생 초본인 꿀풀(Prunella vulgaris Linne var. lilacina Nakai) 또는 하고초(P. vulgaris Linne)의 꽃대이다(대한민국약전, 제11개정, 2017). 하고초는 예로부터 중국, 일본, 한국의 동양의학권 및 유럽에서 민간약으로 널리 사용되었는데, 동양에서는 간경화 및 고혈압에 사용되었고, 유럽에서는 인후 염증 감소, 해열 및 창상 치료 등에 이용되었다. 최근 하고초의 생리활성 연구로는 항알러지, 항염증, 항산화, 항미생물 및 항바이러스 등의 작용이 보고되었다(Psotov et al., 2003).Prunella Spike, on the other hand, is a flowering plant of the perennial herb, Prunella vulgaris Linne var. Lilacina Nakai, or P. vulgaris Linne, belonging to Labiatae (Korean Pharmacopoeia, 11 Amendment, 2017). ). Higocho has been widely used as a folk medicine in China, Japan, Korea, and medicine in Europe. In Asia, it has been used for cirrhosis and hypertension. In Europe, it has been used to reduce throat inflammation, fever and wound treatment. In recent years, physiological activity studies of haejucho were reported to be anti-allergic, anti-inflammatory, antioxidant, antimicrobial and antiviral (Psotov et al., 2003).
이에, 본 발명자들은 오랜 기간 사용되어 인체에 안전한 천연물을 사용하여 황반변성의 치료제를 개발하던 중, 하고초 추출물이 망막색소상피세포 내 A2E 축적을 억제하고, 청색광 유도 망막색소상피세포의 사멸을 억제하며, 청색광 유도 황반변성 동물 모델에서의 시세포 외핵층(outer nuclear layer, ONL) 손상을 억제함을 확인함으로써, 본 발명을 완성하였다.Therefore, the present inventors have been using for a long time, while developing a treatment for macular degeneration using natural products that are safe for human body, the extract of Gojicho inhibits A2E accumulation in retinal pigment epithelial cells, and inhibits the death of blue light induced retinal pigment epithelial cells. The present invention was completed by confirming the inhibition of outer nuclear layer (ONL) damage in an animal model of blue light induced macular degeneration.
본 발명의 목적은 하고초 추출물을 유효성분으로 함유하는 황반변성의 예방, 치료 또는 개선용 조성물을 제공하는 것이다.It is an object of the present invention to provide a composition for the prevention, treatment or improvement of macular degeneration, which contains an extract of Hagocho as an active ingredient.
상기 목적을 달성하기 위하여, 본 발명은 하고초 추출물을 유효성분으로 함유하는 황반변성의 예방 또는 치료용 약학 조성물을 제공한다.In order to achieve the above object, the present invention provides a pharmaceutical composition for the prevention or treatment of macular degeneration, containing the extract of Hagocho as an active ingredient.
또한, 본 발명은 하고초 추출물을 유효성분으로 함유하는 황반변성의 예방 또는 개선용 건강기능식품을 제공한다.The present invention also provides a health functional food for the prevention or improvement of macular degeneration containing the extract of Hagocho as an active ingredient.
본 발명의 하고초 추출물은 망막색소상피세포 내의 A2E 축적을 억제하고, 청색광에 의해 유도된 망막색소상피세포의 사멸을 억제하며, 청색광 유도 황반변성 동물 모델에서 시세포 외핵층의 손상을 억제함으로써, 황반변성 예방, 치료 또는 개선용 조성물로 유용하게 사용될 수 있다.Higocho extract of the present invention inhibits A2E accumulation in retinal pigment epithelial cells, inhibits the death of retinal pigment epithelial cells induced by blue light, and inhibits damage of visual cell outer nucleus layer in blue light induced macular degeneration animal model. It can be usefully used as a composition for preventing, treating or improving sex.
도 1은 하고초 추출물(P.V extract) 및 루테인(Lutein)의 망막색소상피세포 내 A2E 축적 억제 효과를 나타낸 도이다(A2E-BDP: 형광표지된 A2E).
도 2는 하고초 추출물(P.V extract) 및 루테인(Lutein)의 망막색소상피세포 내 A2E 축적 억제 효과를 정량적으로 나타낸 도이다(A2E-BDP: 형광표지된 A2E).
도 3은 하고초 추출물(P.V extract) 및 루테인(Lutein)의 망막색소상피세포 사멸 억제 효과를 나타낸 도이다(BL: 청색광).
도 4는 하고초 추출물의 황반변성 치료 효과를 확인하기 위한 동물실험 일정을 나타낸 도이다.
도 5는 청색광(BL) 유도 황반변성 동물 모델에서의 하고초 추출물(PV) 및 루테인(Lu)의 시세포 외핵층(ONL) 손상 억제 효과를 나타낸 도이다.
도 6은 청색광 유도 황반변성 동물 모델에서의 하고초 추출물(P.V extract) 및 루테인의 시세포 외핵층 손상 억제 효과를 정량적으로 나타낸 도이다.1 is a diagram showing the inhibitory effect of A2E accumulation in retinal pigment epithelial cells of PV extract and Lutein (A2E-BDP: fluorescently labeled A2E).
2 is a quantitative diagram showing the inhibitory effect of A2E accumulation in retinal pigment epithelial cells of PV extract and Lutein (A2E-BDP: fluorescently labeled A2E).
Figure 3 is a diagram showing the effect of inhibiting the retinal pigment epithelial cell death of the extract (PV extract) and lutein (Lutein) (BL: blue light).
Figure 4 is a diagram showing the animal experiment schedule for confirming the macular degeneration treatment effect of Hachocho extract.
FIG. 5 is a diagram showing the effect of inhibiting damage to the cytoplasmic outer nuclear layer (ONL) of Prunella vulgaris (PV) and lutein (Lu) in a blue light (BL) induced macular degeneration animal model.
FIG. 6 is a quantitative diagram showing the effect of inhibiting the damage to the cytocellular extranuclear layer of PV extract and lutein in the blue light induced macular degeneration animal model.
이하, 본 발명을 상세히 설명한다.Hereinafter, the present invention will be described in detail.
본 발명은 하고초 추출물을 유효성분으로 함유하는 황반변성의 예방 또는 치료용 약학 조성물을 제공한다.The present invention provides a pharmaceutical composition for the prevention or treatment of macular degeneration, which contains an extract of Hagocho as an active ingredient.
상기 하고초 추출물은 하기의 단계를 포함하는 제조방법에 의해 제조될 수 있다:The hachoweed extract may be prepared by a manufacturing method comprising the following steps:
1) 하고초에 추출용매를 가하여 추출물을 제조하는 단계;1) preparing an extract by adding an extraction solvent to hacho sec;
2) 단계 1)의 추출물을 여과하는 단계; 및2) filtering the extract of step 1); And
3) 단계 2)의 여과된 여과물을 감압농축한 후 건조하는 단계.3) drying the filtered filtrate of step 2) under reduced pressure.
상기 추출용매는 물, 알코올 또는 이의 혼합물일 수 있다. 상기 알코올은 C1 내지 C4의 저급 알코올일 수 있고, 구체적으로, 상기 저급 알코올은 에탄올 또는 메탄올일 수 있다. 상기 추출용매는 추출에 사용되는 하고초의 중량 1 g당 1 내지 50 mL의 양으로 첨가될 수 있다.The extractant may be water, alcohol or a mixture thereof. The alcohol may be C 1 to C 4 lower alcohol, specifically, the lower alcohol may be ethanol or methanol. The extraction solvent may be added in an amount of 1 to 50 mL per 1 g of the weight of the vinegar used for extraction.
상기 추출방법은 진탕추출, Soxhlet 추출 또는 환류추출일 수 있다. 이때, 추출 시간은 1 내지 50시간, 10 내지 40시간 또는 15 내지 30시간일 수 있다. 상기 추출은 3 내지 5회 반복 추출할 수 있다.The extraction method may be shaking extraction, Soxhlet extraction or reflux extraction. At this time, the extraction time may be 1 to 50 hours, 10 to 40 hours or 15 to 30 hours. The extraction may be repeated 3 to 5 times.
한편, 상기 단계 3)의 감압농축은 진공감압농축기 또는 진공회전증발기를 이용할 수 있다. 또한, 상기 건조는 감압건조, 진공건조, 비등건조, 분무건조 또는 동결건조일 수 있고, 구체적으로는 동결건조일 수 있다.On the other hand, the reduced pressure concentration of step 3) may be used a vacuum pressure reducer or vacuum rotary evaporator. In addition, the drying may be reduced pressure drying, vacuum drying, boiling drying, spray drying or freeze drying, specifically freeze drying.
상기 황반변성은 습성 황반변성 또는 건성 황반변성일 수 있다.The macular degeneration may be wet macular degeneration or dry macular degeneration.
본 발명자들은 하고초 추출물을 제조한 뒤, 상기 하고초 추출물이 망막색소상피세포 내 A2E 축적을 억제하고(도 1 및 2 참조), 청색광으로 유도된 망막색소상피세포의 사멸을 억제함을 확인하였다(도 3 참조). 또한, 하고초 추출물은 청색광으로 유도한 황반변성 동물 모델에서 시세포 외핵층의 손상을 완화시켰다(도 4 및 5 참조). 따라서, 상기 하고초 추출물은 황반변성 예방 또는 치료에 유용하게 사용될 수 있다.The inventors of the present invention, after preparing a hyacinth extract, confirmed that the hyacinth extract inhibits A2E accumulation in retinal pigment epithelial cells (see FIGS. 1 and 2) and inhibits the death of retinal pigment epithelial cells induced by blue light. (See Figure 3). In addition, the Hagocho extract alleviated damage of the extracellular nucleus layer in the macular degeneration animal model induced by blue light (see FIGS. 4 and 5). Therefore, the Hacho herb extract may be usefully used for preventing or treating macular degeneration.
본 발명에 따른 약학 조성물은 조성물 전체 중량에 대하여 유효성분인 하고초 추출물을 10 내지 95 중량%로 포함할 수 있다. 또한, 본 발명의 약학 조성물은 상기 유효성분 이외에 추가로 동일 또는 유사한 기능을 나타내는 유효성분을 1종 이상 추가로 포함할 수 있다.The pharmaceutical composition according to the present invention may include 10 to 95% by weight of the hachocho extract as an active ingredient based on the total weight of the composition. In addition, the pharmaceutical composition of the present invention may further include one or more active ingredients exhibiting the same or similar functions in addition to the active ingredient.
본 발명의 약학 조성물은 생물학적 제제에 통상적으로 사용되는 담체, 희석제, 부형제 또는 이의 혼합물을 포함할 수 있다. 약학적으로 허용가능한 담체는 조성물을 생체 내에 전달하는데 적합한 것이면 모두 사용할 수 있다. 구체적으로, 상기 담체는 Merck Index, 13th ed., Merck & Co. Inc.에 기재된 화합물, 식염수, 멸균수, 링거액, 덱스트로스 용액, 말토덱스트린 용액, 글리세롤, 에탄올 또는 이의 혼합물일 수 있다. 또한, 필요에 따라 항산화제, 완충액, 정균제 등과 같은 통상의 첨가제를 첨가할 수 있다.The pharmaceutical compositions of the present invention may comprise carriers, diluents, excipients or mixtures thereof conventionally used in biological preparations. Pharmaceutically acceptable carriers can be used as long as they are suitable for delivery of the composition in vivo. Specifically, the carrier is Merck Index, 13th ed., Merck & Co. Inc., saline, sterile water, Ringer's solution, dextrose solution, maltodextrin solution, glycerol, ethanol or mixtures thereof. In addition, conventional additives such as antioxidants, buffers, bacteriostatics, etc. may be added as necessary.
상기 조성물을 제제화하는 경우, 보통 사용하는 충진제, 증량제, 결합제, 습윤제, 붕해제, 계면활성제 등의 희석제 또는 부형제를 첨가할 수 있다.When formulating the composition, diluents or excipients such as fillers, extenders, binders, wetting agents, disintegrating agents, surfactants, etc. which are commonly used may be added.
본 발명의 조성물은 경구용 제제 또는 비경구용 제제로 제형화될 수 있다. 경구용 제제로는 고형 제제 및 액상 제제가 포함될 수 있다. 상기 고형 제제는 정제, 환제, 산제, 과립제, 캡슐제 또는 트로키제일 수 있고, 이러한 고형 제제는 상기 조성물에 적어도 하나 이상의 부형제를 첨가하여 조제할 수 있다. 상기 부형제는 전분, 탄산칼슘, 수크로스, 락토오스, 젤라틴 또는 이의 혼합물일 수 있다. 또한, 상기 고형 제제는 윤활제를 포함할 수 있고, 그 예로는 마그네슘 스티레이트, 탈크등이 있다. 한편, 상기 액상 제제는 현탁제, 내용액제, 유제 또는 시럽제일 수 있다. 이때, 상기 액상 제제에는 습윤제, 감미제, 방향제, 보존제 등과 같은 부형제가 포함될 수 있다.The composition of the present invention may be formulated as an oral or parenteral preparation. Oral formulations may include solid and liquid formulations. The solid preparation may be tablets, pills, powders, granules, capsules or troches, and such solid preparations may be prepared by adding at least one excipient to the composition. The excipient may be starch, calcium carbonate, sucrose, lactose, gelatin or mixtures thereof. In addition, the solid preparation may include a lubricant, for example magnesium styrate, talc and the like. On the other hand, the liquid formulation may be a suspension, a liquid solution, an emulsion or a syrup. At this time, the liquid formulation may include excipients such as wetting agents, sweeteners, fragrances, preservatives and the like.
상기 비경구용 제제는 주사제, 좌제, 호흡기 흡입용 분말, 스프레이용 에어로졸제, 파우더 및 크림 등을 포함할 수 있다. 상기 주사제는 멸균된 수용액, 비수성용제, 현탁용제, 유제 등을 포함할 수 있다. 이때, 비수성용제 또는 현탁용제로서는 프로필렌글리콜, 폴리에틸렌글리콜, 올리브 오일과 같은 식물성 기름이나, 에틸올레이트와 같이 주사가능한 에스테르 등이 사용될 수 있다.The parenteral preparations may include injections, suppositories, respiratory inhalation powders, spray aerosols, powders and creams, and the like. The injection may include a sterile aqueous solution, a non-aqueous solvent, a suspension solvent, an emulsion, and the like. In this case, as the non-aqueous solvent or suspending solvent, vegetable oil such as propylene glycol, polyethylene glycol, olive oil, or injectable ester such as ethyl oleate may be used.
본 발명의 조성물은 목적하는 방법에 따라 경구 또는 비경구로 투여될 수 있다. 비경구 투여는 복강내, 직장내, 피하, 정맥, 근육내 또는 흉부내 주사 방식을 포함할 수 있다.The composition of the present invention can be administered orally or parenterally according to the desired method. Parenteral administration can include intraperitoneal, rectal, subcutaneous, intravenous, intramuscular or intrathoracic injection modes.
상기 조성물은 약학적으로 유효한 양으로 투여될 수 있다. 이는 질환의 종류, 중증도, 약물의 활성, 약물에 대한 환자의 민감도, 투여 시간, 투여 경로, 치료기간, 동시에 사용되는 약물 등에 따라 달라질 수 있다. 그러나, 바람직한 효과를 위해서, 본 발명에 따른 약학 조성물에 포함되는 유효성분의 양은 0.0001 내지 100 ㎎/㎏, 구체적으로 0.001 내지 10 ㎎/㎏일 수 있다. 상기 투여는 하루에 1회 내지 수회일 수 있다.The composition may be administered in a pharmaceutically effective amount. This may vary depending on the type of disease, the severity, the activity of the drug, the patient's sensitivity to the drug, the time of administration, the route of administration, the duration of treatment, the drug being used simultaneously, and the like. However, for the desired effect, the amount of the active ingredient included in the pharmaceutical composition according to the present invention may be 0.0001 to 100 mg / kg, specifically 0.001 to 10 mg / kg. The administration can be from one to several times a day.
본 발명의 조성물은 단독 또는 다른 치료제와 병용하여 투여될 수 있다. 병용 투여시, 투여는 순차적 또는 동시일 수 있다.The composition of the present invention may be administered alone or in combination with other therapeutic agents. In combination administration, administration may be sequential or simultaneous.
또한, 본 발명은 하고초 추출물을 유효성분으로 함유하는 황반변성의 예방 또는 개선용 건강기능식품을 제공한다.The present invention also provides a health functional food for the prevention or improvement of macular degeneration containing the extract of Hagocho as an active ingredient.
상기 하고초 추출물은 하고초에 추출용매를 가하여 추출물을 제조하고, 그 추출물을 여과한 후, 이를 감압농축하고 건조하는 단계를 포함하는 제조방법에 의해 제조될 수 있다.The extract of Hagocho may be prepared by adding an extraction solvent to Hagocho to prepare an extract, and filtering the extract, followed by concentration under reduced pressure and drying.
상기 추출용매는 물, 알코올 또는 이의 혼합물일 수 있다. 상기 알코올은 C1 내지 C4의 저급 알코올일 수 있고, 구체적으로, 상기 저급 알코올은 에탄올 또는 메탄올일 수 있다. 상기 추출용매는 추출에 사용되는 하고초의 중량 1 g당 1 내지 50 mL의 양으로 첨가될 수 있다.The extractant may be water, alcohol or a mixture thereof. The alcohol may be C 1 to C 4 lower alcohol, specifically, the lower alcohol may be ethanol or methanol. The extraction solvent may be added in an amount of 1 to 50 mL per 1 g of the weight of the vinegar used for extraction.
상기 황반변성은 습성 황반변성 또는 건성 황반변성일 수 있다.The macular degeneration may be wet macular degeneration or dry macular degeneration.
본 발명자들은 하고초 추출물을 제조한 뒤, 상기 하고초 추출물이 망막색소상피세포 내 A2E 축적을 억제하고(도 1 및 2 참조), 청색광으로 유도된 망막색소상피세포의 사멸을 억제함을 확인하였다(도 3 참조). 또한, 하고초 추출물은 청색광으로 유도한 황반변성 동물 모델에서 시세포 외핵층의 손상을 완화시켰다(도 4 및 5 참조). 따라서, 상기 하고초 추출물은 황반변성 예방 또는 개선에 유용하게 사용될 수 있다.The inventors of the present invention, after preparing a hyacinth extract, confirmed that the hyacinth extract inhibits A2E accumulation in retinal pigment epithelial cells (see FIGS. 1 and 2) and inhibits the death of retinal pigment epithelial cells induced by blue light. (See Figure 3). In addition, the Hagocho extract alleviated damage of the extracellular nucleus layer in the macular degeneration animal model induced by blue light (see FIGS. 4 and 5). Therefore, the Hacho herb extract may be usefully used for preventing or improving macular degeneration.
본 발명의 조성물은 식품에 그대로 첨가하거나, 다른 식품 또는 식품 성분과 함께 사용될 수 있다. 이때, 첨가되는 유효성분의 함량은 목적에 따라 결정될 수 있고, 일반적으로는 전체 식품 중량의 0.01 내지 90 중량부일 수 있다.The composition of the present invention may be added as it is to food, or used with other foods or food ingredients. In this case, the amount of the active ingredient added may be determined according to the purpose, and generally may be 0.01 to 90 parts by weight of the total food weight.
건강기능식품의 형태 및 종류는 특별히 제한되지 않는다. 구체적으로, 상기 건강기능식품은 정제, 캅셀, 분말, 과립, 액상 및 환의 형태일 수 있다. 상기 건강기능식품은 추가성분으로서 여러 가지 향미제, 감미제 또는 천연 탄수화물을 포함할 수 있다. 상기 감미제는 천연 또는 합성 감미제일 수 있고, 천연 감미제의 예로는 타우마틴, 스테비아 추출물 등이 있다. 한편, 합성 감미제의 예로는 사카린, 아스파르탐 등이 있다. 또한, 상기 천연 탄수화물은 모노사카라이드, 디사카라이드, 폴리사카라이드, 올리고당 및 당알코올 등일 수 있다.The form and type of dietary supplement are not particularly limited. Specifically, the health functional food may be in the form of tablets, capsules, powders, granules, liquids and pills. The dietary supplement may include various flavors, sweeteners or natural carbohydrates as additional ingredients. The sweetener may be a natural or synthetic sweetener, and examples of the natural sweetener include taumartin, stevia extract, and the like. On the other hand, examples of the synthetic sweeteners include saccharin, aspartame, and the like. In addition, the natural carbohydrate may be monosaccharides, disaccharides, polysaccharides, oligosaccharides and sugar alcohols.
본 발명의 건강기능식품은 상기 서술한 추가성분 외에, 영양제, 비타민, 전해질, 풍미제, 착색제, 펙스탄 및 그의 염, 알긴산 및 그의 염, 유기산, 보호성 콜로이드 증점제, pH 조절제, 안정화제, 방부제, 글리세린, 알코올 등을 더 포함할 수 있다. 이러한 성분은 독립적으로 또는 조합으로 사용될 수 있다. 상기 첨가제의 비율은 본 발명의 조성물의 100 중량부당 0.01 내지 0.1 중량부의 범위에서 선택될 수 있다.In addition to the above-mentioned additional ingredients, the health functional food of the present invention is a nutrient, vitamin, electrolyte, flavoring agent, coloring agent, pectane and salt thereof, alginic acid and salt thereof, organic acid, protective colloid thickener, pH adjusting agent, stabilizer, and preservative. , Glycerin, alcohol, and the like may be further included. These components can be used independently or in combination. The proportion of the additive may be selected in the range of 0.01 to 0.1 parts by weight per 100 parts by weight of the composition of the present invention.
이하, 본 발명을 하기 실시예에 의해 상세히 설명한다.Hereinafter, the present invention will be described in detail by the following examples.
단, 하기 실시예는 본 발명을 예시하기 위한 것일 뿐, 본 발명이 이들에 의해 한정되는 것은 아니다.However, the following Examples are only for illustrating the present invention, and the present invention is not limited thereto.
실시예 1. 하고초 추출물의 제조Example 1 Preparation of Seaweed Extract
건조된 꿀풀(Prunella vulgaris var. lilacina)의 꽃대 부분(Lot No. JH123-140203, 조화제약)을 분쇄한 후, 증류수를 100 g/L의 비율로 첨가하고 100℃에서 2시간 동안 추출하였다. 추출액을 여과한 후에 회전농축기를 이용하여 농축시킨 후, 동결 건조하였다.After crushing the stalk portion (Lot No. JH123-140203, Harmonic Pharmaceuticals) of dried nectar ( Prunella vulgaris var. Lilacina), distilled water was added at a rate of 100 g / L and extracted at 100 ° C for 2 hours. The extract was filtered, concentrated using a rotary concentrator, and freeze-dried.
실험예 1. 하고초 추출물의 망막색소상피세포 내 A2E 축적 억제 효과Experimental Example 1. Inhibitory effect of A2E accumulation on retinal pigment epithelial cells
망막색소상피세포의 A2E 축적은 황반변성의 발생에 주요 역할을 하므로, 하고초 추출물이 망막색소상피세포 내 A2E 축적을 억제하는 효과가 있는지 확인하기 위하여, 인간 망막색소상피세포주인 ARPE-19세포 및 형광표지된 A2E를 이용하였다.Since A2E accumulation of retinal pigment epithelial cells plays a major role in the development of macular degeneration, in order to determine whether the extract of Higocho has an effect of inhibiting A2E accumulation in retinal pigment epithelial cells, human retinal pigment epithelial cell line ARPE-19 cells and fluorescence Labeled A2E was used.
구체적으로, ARPE-19세포(American Type Culture Collection, 미국)에 상기 실시예 1에서 수득한 하고초 추출물 0, 25, 50, 100 또는 200 ㎍/mL 또는 루테인 17.04 ㎍/mL (30 μM)을 처리한 다음, 형광표지된 A2E(A2E-BDP) 20 μM을 ARPE-19세포에 처리하고, 24시간 뒤에 상층액을 제거한 후, 인산염 완충액(phosphate buffered saline, PBS)으로 세척하였다. 상기 ARPE-19세포를 형광현미경(Nikon Eclipse Ti-U Fluorescence, 일본)으로 관찰하고, 형광광도계(FLUOstar Omega, BMG Labtech, 미국)로 형광을 측정하여 세포 내 축적된 A2E를 정량하였다.Specifically, ARPE-19 cells (American Type Culture Collection, USA) were treated with the
그 결과, 루테인 처리군에서는 A2E 축적을 유도한 음성대조군에 비하여 세포 내 A2E 축적을 25% 억제한 반면, 하고초 추출물은 25, 50, 100 또는 200 ㎍/mL 처리군에서 A2E 축적을 각각 13, 20, 37 또는 49% 억제하였다(도 1 및 2). 이는 하고초 추출물 100 ㎍/mL 이상 처리군이 루테인 17.04 ㎍/mL(30 μM) 처리군보다 우수한 세포 내 A2E 축적 억제 효과를 가짐을 제시한다.As a result, the lutein-treated group inhibited A2E accumulation in cells by 25% compared to the negative control group that induced A2E accumulation, whereas the Higocho extract inhibited A2E accumulation in 25, 50, 100 or 200 ㎍ / mL treated groups by 13, 20, 37 or 49% inhibition (FIGS. 1 and 2). This suggests that the treatment group of 100 μg / mL or more of the Hagocho extract has a superior inhibitory effect on A2E accumulation in cells than the lutein 17.04 μg / mL (30 μM) treatment group.
실험예 2. 하고초 추출물의 청색광 유도 광산화에 대한 망막색소상피세포 보호 효과Experimental Example 2. Protective effect of retinal pigment epithelial cells on blue light induced photooxidation
망막색소상피세포에 축적된 A2E는 청색광 조사 시 광산화가 일어나 세포독성을 유발하는 것으로 알려져 있는 바, ARPE-19세포에 A2E 축적 후 청색광을 조사하여 유발되는 세포독성을 하고초 추출물이 억제할 수 있는지 확인하였다.It is known that A2E accumulated in retinal pigment epithelial cells causes cytotoxicity when blue light is irradiated, and it is cytotoxic caused by irradiation of blue light after A2E accumulation in ARPE-19 cells. Confirmed.
구체적으로, ARPE-19세포에 상기 실시예 1에서 수득한 하고초 추출물 0, 25, 50, 100 또는 200 ㎍/mL 또는 루테인 17.04 ㎍/mL(30 μM)을 24시간 동안 처리한 다음, A2E 20 μM을 24시간 동안 처리하고, 청색광(4,000 lux)을 10분 동안 조사하였다. 이후, ARPE-19세포의 세포생존율을 셀 카운팅 키트(cell counting kit, Dojindo Labs, 일본)로 측정하였으며, A2E를 축적시키고, 청색광을 조사하지 않은 대조군에 대한 각 처리군의 세포생존율을 백분율(%)로 나타내었다(도 3).Specifically, ARPE-19 cells were treated with the
그 결과, A2E를 축적시키고, 청색광을 조사한 음성대조군의 세포생존율이 대조군 대비 유의하게 감소하여 세포사멸이 유도되었다. 대조군과 음성대조군의 세포생존율 차이를 100%로 하여 각 약물의 세포 보호 효과를 계산한 결과, 루테인의 세포 보호 효과는 53%, 하고초 추출물의 세포 보호 효과는 25, 50, 100 또는 200 ㎍/mL 처리군에서 각각 34.8, 48.6, 62.1 또는 69.5%였다(도 3). 이는, 하고초 추출물 100 ㎍/mL 이상 처리군이 루테인 17.04 ㎍/mL(30 μM) 처리군보다 우수한 세포 보호 효과를 가짐을 제시한다.As a result, apoptosis was induced as A2E was accumulated and the cell viability of the negative control group irradiated with blue light was significantly reduced compared to the control group. The cell protection effect of each drug was calculated using the difference in cell viability of the control group and the negative control group as 100%, and the cell protection effect of lutein was 53%, and the cell protection effect of the haejucho extract was 25, 50, 100 or 200 ㎍ /. 34.8, 48.6, 62.1 or 69.5%, respectively, in the mL treatment group (FIG. 3). This suggests that the treatment group of 100 μg / mL or more of the Hagocho extract has a superior cell protective effect than the lutein 17.04 μg / mL (30 μM) treatment group.
실험예 3. 하고초 추출물의 청색광 유도 황반변성 억제 효과Experimental Example 3 Inhibitory Effect of Extracts from Hagocho on Blue Light Induced Macular Degeneration
상기 실험예 1 및 2에서 확인한 하고초 추출물의 망막색소상피세포 보호 효과를 동물 모델에서 검증하기 위하여, 청색광으로 유도한 황반변성 동물 모델에서 하기와 같은 실험을 수행하였다.In order to verify the protective effect of retinal pigment epithelial cells of the haejucho extract confirmed in Experimental Examples 1 and 2 in an animal model, the following experiment was performed in the macular degeneration animal model induced by blue light.
3-1. 황반변성 동물 모델의 준비 및 실험 일정3-1. Preparation and Experimental Schedule of Macular Degeneration Animal Models
5주령의 BALB/C 마우스를 2일간 순화사육 후, 상기 실시예 1에서 수득한 하고초 추출물(50, 100 또는 200 mg/kg) 또는 루테인(100 mg/kg)을 5일간 매일 1회씩 투여하였다. 이후, 24시간 암순응을 거치고, 14일 동안 청색광을 10,000 lux로 매일 1시간씩 조사하면서 청색광 조사 10분전마다 상기 하고초 추출물(50, 100 또는 200 mg/kg) 또는 루테인(100 mg/kg)을 투여하였다. 청색광 조사 및 약물 투여 종료 후 7일 뒤에 마우스를 희생시켜 안구를 적출하고 하고초 추출물의 망막 시세포 보호 효과를 분석하였다.After 5 weeks old BALB / C mice were incubated for 2 days, the haecho extract (50, 100 or 200 mg / kg) or lutein (100 mg / kg) obtained in Example 1 was administered once daily for 5 days. . Thereafter, after 24 hours of dark acclimatization, the haegocho extract (50, 100 or 200 mg / kg) or lutein (100 mg / kg) was applied every 10 minutes before the blue light irradiation while irradiating blue light at 10,000 lux for 1 hour every day for 14 days. Administered. Seven days after the end of blue light irradiation and drug administration, mice were sacrificed to extract eyeballs, and the retinal progenitor protective effect was analyzed.
3-2. 하고초 추출물의 망막 시세포 보호 효과3-2. Protective Effect of Rhizome Extracts on Retinal Cells
적출한 안구 조직을 중성 완충 포르말린 용액(neutral buffered formalin)에 고정하고, 세척한 후, 알코올을 이용하여 탈수 과정을 거치고, 자일렌(xylene)을 이용하여 투명 과정을 진행한 뒤에, 파라핀으로 포매하였다. 포매된 조직 블록을 4 ㎛ 두께로 삭정(trimming)하여 조직 절편을 제작한 후, 헤마톡실린 & 에오신(hematoxylin & eosin, H & E) 염색을 수행하였다. 구체적으로, 조직 절편에 헤마톡실린을 30초간 처리하고, 10분간 수세한 후, 에오신을 1분간 처리하였다. 현미경(Olympus Optical, 일본)으로 염색된 안구 조직 절편의 사진을 찍은 뒤, 이미지 J 소프트웨어(Image J software, National Institute of Health, 미국)로 시신경에서부터 600 ~ 900 ㎛에 위치한 부위에서 시세포 외핵층의 두께를 측정하고 핵 수를 카운팅하였다.The extracted ocular tissues were fixed in neutral buffered formalin, washed, dehydrated with alcohol, transparent with xylene, and embedded in paraffin. . Tissue sections were prepared by trimming the embedded tissue block to 4 μm thickness, followed by hematoxylin & eosin (H & E) staining. Specifically, the tissue sections were treated with hematoxylin for 30 seconds, washed with water for 10 minutes, and then treated with eosin for 1 minute. Photographs of ocular tissue sections stained with a microscope (Olympus Optical, Japan), followed by image J software (Image J software, National Institute of Health, USA) thickness of the extracellular nucleus layer at 600-900 μm from the optic nerve Was measured and the number of nuclei was counted.
시세포 외핵층의 두께 측정 결과, 청색광을 조사하지 않은 대조군에 비하여 청색광을 조사한 음성대조군에서 유의하게 감소하였으며, 하고초 추출물 또는 루테인 투여군에서 음성대조군 대비 유의하게 증가하였다. 대조군과 음성대조군의 시세포 외핵층 두께 차이를 100%로 하여 각 약물 투여군의 음성대조군에 대한 시세포 외핵층 두께 차이를 계산한 결과, 루테인 투여군은 49.1%, 하고초 추출물 투여군은 50, 100 또는 200 mg/kg 투여군에서 각각 35.8, 50.5 또는 71.2%로 나타났다(도 5 및 6).As a result of the measurement of the thickness of the cell outer core layer, it was significantly decreased in the negative control group irradiated with blue light compared to the control group not irradiated with blue light, and significantly increased in the negative control group in the Pleurotus chinensis extract or lutein administration group. As a result of calculating the difference in the thickness of the extracellular nuclear layer in the negative control group of the control group and the negative control group as 100%, 49.1% in the lutein group and the 50, 100, or 200 mg in the plethyrum extract group 35.8, 50.5 or 71.2% in the / kg administration group, respectively (Figs. 5 and 6).
시세포 외핵층의 핵 수를 측정한 결과, 청색광을 조사하지 않은 대조군에 비하여 청색광을 조사한 음성대조군에서 유의하게 감소하였으며, 하고초 추출물 또는 루테인 투여군에서 음성대조군 대비 유의하게 증가하였다. 대조군과 음성대조군의 시세포 외핵층 핵 수 차이를 100%로 하여 각 약물 투여군의 음성대조군에 대한 시세포 외핵층 핵 수 차이를 계산한 결과, 루테인 투여군은 29.3%, 하고초 추출물 투여군은 50, 100 또는 200 mg/kg 투여군에서 각각 31.6, 33.9 또는 50.8%로 나타났다(도 5 및 7).As a result of measuring the number of nuclei of the cell nucleus layer, it was significantly decreased in the negative control group irradiated with blue light compared to the control group not irradiated with blue light, and significantly increased in the negative control group in the pleated vinegar extract or lutein administration group. As a result of calculating the difference in cell number in the nuclear cell layer of the negative control group of the control group and the negative control group as 100%, the lutein-treated group was 29.3%, the pleated extract group was 50, 100 or In the 200 mg / kg administration group was 31.6, 33.9 or 50.8%, respectively (Figs. 5 and 7).
이는 청색광 유도 황반변성 모델에서, 하고초 추출물이 루테인과 유사한 수준으로 망막 시세포 손상을 유의하게 회복시키는 효과가 있음을 제시한다.This suggests that, in the blue light induced macular degeneration model, the hydrangea extract has an effect of significantly repairing retinal cell damage at levels similar to lutein.
결론적으로, 상기 실시예 및 실험예를 통하여, 하고초 추출물이 우수한 망막색소상피세포 내 A2E 축적 억제, 청색광 유도 망막색소상피세포 독성에 대한 보호 효과 및 청색광 유도 황반변성에 대한 억제 효과를 보임을 확인하였다. 따라서, 하고초 추출물은 황반변성 예방, 치료 또는 개선에 유용하게 사용될 수 있다.In conclusion, it was confirmed from the above examples and experimental examples that the Hagocho extract showed excellent inhibition of A2E accumulation in retinal pigment epithelial cells, protection against blue light-induced retinal pigment epithelial cell toxicity, and blue light induced macular degeneration. . Therefore, Hachocho extract can be usefully used for preventing, treating or improving macular degeneration.
Claims (8)
A pharmaceutical composition for the prevention or treatment of macular degeneration, containing the extract of Hagocho as an active ingredient.
The pharmaceutical composition of claim 1, wherein the extract is extracted with water, C 1 to C 4 lower alcohols, or a mixed solvent thereof.
The pharmaceutical composition of claim 2, wherein the lower alcohol is ethanol or methanol.
The pharmaceutical composition of claim 1, wherein the macular degeneration is wet macular degeneration or dry macular degeneration.
Health functional food for the prevention or improvement of macular degeneration containing the extract of Hagocho as an active ingredient.
The health functional food according to claim 5, wherein the extract is extracted with water, C 1 to C 4 lower alcohols, or a mixed solvent thereof.
The dietary supplement of claim 6, wherein the lower alcohol is ethanol or methanol.
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