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Hyeong-Geug Kim,Seong-Soon Jang,Jin-Seok Lee,Hyo-Seon Kim,Chang-Gue Son 고려인삼학회 2017 Journal of Ginseng Research Vol.41 No.2
Background: Radiotherapy is one of the most important modalities in cancer treatment; however, normal tissue damage is a serious concern. Drug development for the protection or reduction of normal tissue damage is therefore a clinical issue. Herein, we evaluated the protective properties of Panax ginseng Meyer and its corresponding mechanisms. Methods: C56BL/6 mice were orally pretreated with P. ginseng water extract (PGE; 25 mg/kg, 50 mg/kg, or 100 mg/kg) or intraperitoneally injected melatonin (20 mg/kg) for 4 d consecutively, then exposed to 15-Gy X-ray radiation 1 h after the last administration. After 10 d of irradiation, the biological properties of hematoxicity, fat accumulation, histopathology, oxidative stress, antioxidant activity, proinflammatory cytokines, and apoptosis signals were examined in the hepatic tissue. Results: The irradiation markedly induced myelosuppression as determined by hematological analysis of the peripheral blood. Steatohepatitis was induced by X-ray irradiations, whereas pretreatment with PGE significantly attenuated it. Oxidative stress was drastically increased, whereas antioxidant components were depleted by irradiation. Irradiation also notably increased serum liver enzymes and hepatic protein levels of pro-inflammatory cytokines. Those alterations were markedly normalized by pretreatment with PGE. The degree of irradiation-induced hepatic tissue apoptosis was also attenuated by pretreatment with PGE, which was evidenced by a terminal deoxynucleotidyl transferase 20-deoxyuridine 50-triphosphate nick-end labeling assay, western blotting, and gene expressions analysis, particularly of apoptotic molecules. Conclusion: We suggest that PGE could be applicable for use against radiation-induced liver injury, and its corresponding mechanisms involve the modulation of oxidative stress, inflammatory reactions, and apoptosis.
Hyeong Seok Jang(장형석),Nam Seon Kang(강남선),Kyeong Mi Kim(김경미),Byung Hee Jeon(전병희),Joon Sang Park(박준상),Ji Won Hong(홍지원) 한국생명과학회 2017 생명과학회지 Vol.27 No.10
단세포 녹조류 균주를 경상북도 울릉군 울릉도 거북바위 주변 조수웅덩이로부터 순수분리하여 형태적, 분자적, 및 생화학적 특성을 분석한 결과 옥세노클로렐라 프로토테코이드에 속하는 것으로 밝혀졌다. 본 종은 현재까지 한국에서 공식 기록이 없는 미기록종으로 옥세노클로렐라 프로토테코이드 MM0011 균주라고 명명하였으며, 생장, 지질/광합성 색소 조성 및 바이오매스 특성에 대해 조사를 실시하였다. 분리균주는 광범위한 온도(5-35°C)에서 생장할 수 있었으며 1.5 M 염화나트륨 농도까지 생존할 수 있었다. 가스크로마토그래프/질량분석기를 이용한 분석 결과, 본 균주에는 영양적으로 중요한 불포화지방산이 풍부한 것으로 나타났으며, 특히 리놀네산(27.6%) 및 알파 리놀렌산(37.2%)이 주요 지방산 성분으로 확인되었다. 따라서 본 토착 미세조류 균주는 어유 또는 식물성유를 대체할 수 있는 잠재적인 오메가-3 및 오메가-6 불포화지방산 원료가 될 수 있을 것으로 사료된다. 또한, 고부가가치 항산화 물질인 루테인이 보조색소로서 본 균주에 의해 생합성 되는 것으로 밝혀졌다. 일반성분분석 결과 MM0011 균주의 휘발성물질 함량은 85.6%였으며, 원소분석 결과 총 발열량은 20.3 MJ kg<SUP>-1</SUP>으로 나타났다. 또한 배지로부터 40.5%의 전질소와 27.9%의 전인을 각각 제거할 수 있어 향후 바이오연료 원료물질 생산과 오 · 폐수처리를 연계할 수 있는 가능성 역시 제시하였다. 추가적으로 MM0011 바이오매스는 높은 단백질 함량(51.4%)을 갖고 있어 우수한 동물사료의 원료가 될 수 있는 가능성도 보여주고 있다. 따라서, 본 균주는 미세조류 기반 생화학 물질 생산 및 바이오매스 원료로서 상업적인 이용 가능성이 높음을 시사한다. A unicellular green alga was axenically isolated from a tidal pool on Ulleung-do, Korea. Morphological, molecular, and biochemical analyses revealed that the isolate belonged to Auxenochlorella protothecoides. The current study is the first record of this species in Korea. The microalgal strain was named as A. protothecoides MM0011 and its growth, lipid and pigment compositions, and biomass properties were investigated. The strain is able to thrive in a wide range of temperatures (5~35°C) and to withstand up to 1.5 M NaCl. The results of GC/MS analysis showed that the isolate was rich in nutritionally important polyunsaturated fatty acids (PUFAs). Its major fatty acids were linoleic acid (27.6%) and α -linolenic acid (39.6%). Thus, this indigenous microalga has potential as an alternative source of ω3 and ω6 PUFAs, which currently come from fish and plant oils. Also, the HPLC analysis revealed that the value-added antioxidant, lutein, was biosynthesized as the accessory pigments by the microalga. A proximate analysis showed that the volatile matter content was 85.6% and an ultimate analysis indicated that the gross calorific value was 20.3 MJ kg<SUP>-1</SUP>. Since 40.5% of total nitrogen and 27.9% of total phosphorus were removed from the medium, respectively, it also has potential as a feedstock for biofuel applications which could be coupled to wastewater treatment. In addition, the biomass may also serve as an excellent animal feed because of its high protein content (51.4%). Therefore, A. protothecoides MM0011 shows promise for application in production of microalgae-based biochemicals and as a biomass feedstock.
( Hyeong In Kim ),( Dong Lim Seol ),( Min Young Choi ),( Ji Yeon Seo ),( Young Chul Yoon ),( Soon Ho Cheong ),( Ki Jung Ahn ),( Mi Seon Kang ),( Won Hee Jang ),( Young Il Yang ) 한국조직공학·재생의학회 2009 조직공학과 재생의학 Vol.6 No.1
Ionizing radiation produces both acute and delayed effects on skin and subcutaneous tissues, resulting in profound impairment in wound healing. Adipose tissue-derived stem cells(ASCs) have the potential to differentiate into different cell lineages and could be used to repair numerous injured tissues. We examined whether intradermal injection of ASCs would improve the impaired wound healing in irradiated mice. Mice were locally irradiated to the hindlimb to induce radiation dermatitis. Four weeks after irradiation, syngeneic ASCs were delivered into intradermal area of irradiated skin. To assess the effect of the ASCs injection, phenotypic and morphologic analyses and blood flow rate were assessed. The phenotypic analysis showed a progression from erythema to ulceration in irradiated mice. However, irradiated mice injected with ASCs displayed a complete healing of the epidermis and restoration of dermal components. CD31+ microvessels were significantly increased in irradiated mice injected with ASCs compared to those injected with PBS(p<0.05). Inaddition, blood flow rate was higher in irradiated mice injected with ASCs than those injected with PBS(p<0.01). The injected ASCs mostly located in dermis and formed vimentin-positive stromal cells. A few injected ASCs were incorporated into microvasculatures. In conclusion, ASCs could be used as useful cell therapeutics to accelerate wound healing in radiation-induced tissue damage.
Kim, Hyeong-Geug,Jang, Seong-Soon,Lee, Jin-Seok,Kim, Hyo-Seon,Son, Chang-Gue The Korean Society of Ginseng 2017 Journal of Ginseng Research Vol.41 No.2
Background: Radiotherapy is one of the most important modalities in cancer treatment; however, normal tissue damage is a serious concern. Drug development for the protection or reduction of normal tissue damage is therefore a clinical issue. Herein, we evaluated the protective properties of Panax ginseng Meyer and its corresponding mechanisms. Methods: C56BL/6 mice were orally pretreated with P. ginseng water extract (PGE; 25 mg/kg, 50 mg/kg, or 100 mg/kg) or intraperitoneally injected melatonin (20 mg/kg) for 4 d consecutively, then exposed to 15-Gy X-ray radiation 1 h after the last administration. After 10 d of irradiation, the biological properties of hematoxicity, fat accumulation, histopathology, oxidative stress, antioxidant activity, pro-inflammatory cytokines, and apoptosis signals were examined in the hepatic tissue. Results: The irradiation markedly induced myelosuppression as determined by hematological analysis of the peripheral blood. Steatohepatitis was induced by X-ray irradiations, whereas pretreatment with PGE significantly attenuated it. Oxidative stress was drastically increased, whereas antioxidant components were depleted by irradiation. Irradiation also notably increased serum liver enzymes and hepatic protein levels of pro-inflammatory cytokines. Those alterations were markedly normalized by pretreatment with PGE. The degree of irradiation-induced hepatic tissue apoptosis was also attenuated by pretreatment with PGE, which was evidenced by a terminal deoxynucleotidyl transferase 2'-deoxyuridine 5'-triphosphate nick-end labeling assay, western blotting, and gene expressions analysis, particularly of apoptotic molecules. Conclusion: We suggest that PGE could be applicable for use against radiation-induced liver injury, and its corresponding mechanisms involve the modulation of oxidative stress, inflammatory reactions, and apoptosis.