• 한국산학기술학회논문지
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• 제14권11호
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• pp.5646-5657
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• 2013

본 연구에서는 뽕잎차와 Monascus pilosus로 발효시킨 뽕잎차가 ICR mouse의 체중과 간 조직 항산화계 효소류의 활성에 미치는 영향을 조사하고자 음용수 대신 1% 열수 추출액을 8주간 급여하고 체중, 장기중량, 혈액 및간기능 바이오 마커들의 변화를 관찰하였다. Mice는 뽕잎차(UMI)와 발효뽕잎차의 열수추출액 급여군(FMI) 및 정상대조군(NC) 등 3개군으로 나누었다. 차 추출액을 급여한 군들은 유의한 차이는 보이지 않았으나 NC군에 비하여 체중 증가량이 감소하였고, LDL-콜레스테롤, 동맥경화 지수는 유의한 수준의 감소를 보였으며, 간 조직의 lipid peroxide (LPO) 함량 및 xanthin oxidase (XO) 활성의 감소와 glutathione S-transferase (GST) 활성의 유의적인 증가를 관찰할 수 있었다. 이상의 실험결과, 뽕잎차 및 M. pilosus로 발효시킨 뽕잎차는 체중감소 효과가 있으며 간 조직 손상과 관련된 항산화계 효소의 활성을 높여주는 효과가 있는 것으로 사료된다.

• Journal of Microbiology and Biotechnology
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• 제28권7호
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• pp.1199-1208
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• 2018

Osteoarthritis is a disease that affects the articular cartilage and osseous tissue, and can be worsened by aging, overweight status, and post-traumatic arthritis. The present study aimed to evaluate the effect of ID-CBT5101 (tyndallized Clostridium butyricum) on bone metabolism and the inflammatory response in a monosodium iodoacetate-induced rat model of osteoarthritis. ID-CBT5101 was administered orally at doses of $10^8$ or $10^{10}CFU/day$ for 2 weeks before direct injection of monosodium iodoacetate ($3mg/50{\mu}l$ of 0.9% saline) into the intra-articular space of the rats' right knees. The rats subsequently received the same doses of oral ID-CBT5101 for another 4 weeks. We evaluated the treatment effects based on serum biomarkers, mRNA expression, morphological and histopathological analyses of the knee joints, and weight-bearing distribution analysis. Compared with those in control rats, the ID-CBT5101 treatments significantly reduced the serum concentration of inflammation and bone metabolism markers (i.e., COX-2, IL-6, $LTB_4$, and COMP), and significantly increased the concentration of $IFN-{\gamma}$ and glycosaminoglycans. In addition, the ID-CBT5101 treatments inhibited the mRNA expression of matrix metalloproteinases and tissue inhibitors of metalloproteinases (i.e., MMP-2, MMP-3, MMP-9, MMP-13, TIMP-1, and TIMP-2). Furthermore, the ID-CBT5101 treatments effectively preserved the knee cartilage and synovial membrane, and significantly decreased the amount of fibrous tissue. Moreover, compared with that of the negative control group, the ID-CBT5101 treatments increased the weight-bearing distribution by ${\geq}20%$. The results indicate that ID-CBT5101 prevented and alleviated osteoarthritis symptoms. Thus, ID-CBT5101 may be a novel therapeutic option for the management of osteoarthritis.

• 한국작물학회지
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• 제59권3호
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• pp.252-262
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• 2014

혈당 강하를 목적으로 선발된 수수계통의 종자 유래 펩타이드의 양적, 질적 형질을 특성화하고 혈당 강하 수수에서 특이적으로 발현 펩타이드를 선발하기 위하여, 혈당 강하수수 7계통과 비 혈당 강하 수수 5계통에 대한 종자 펩타이드 프로파일링을 SELDI-TOF MS 기법을 활용하여 분석하였다. 1. 분자량의 범위가 2~20 kDa에서 검출된 수수 12계통 종자의 펩타이드는 CM10 (weak cation exchanger)에서 104개와 Q10 (strong anion exchanger)에서 95개였으며, 펩타이드 양적발현에서 12계통 간 유의성(p < 0.01)을 보인 펩타이드는 CM10에서 99개와 Q10에서 93개였다. 2. 12계통 간 양적 발현에 유의적(p < 0.01) 펩타이드를 이용한 heat map 분석에서 수수 각 계통 종자의 고유한 펩타이드 프로파일과 특이적으로 발현하는 펩타이드를 제시하고 있다. 3. 수수 12계통간의 근연거리를 이용한 군집분석에서 혈당 강하 수수 7계통과 비 혈당 강하 수수 5계통이 서로 다른 2개의 군집을 형성하였다. 4. 혈당 강하 계통에서 유의성(p < 0.00001)이 있게 발현되는 펩타이드를 29개 선정하였으며, 이중에서 혈당강하 계통에서만 공통적으로 높게 발현된 10개의 펩타이드(분자량이 2231.6, 2845.4, 2907.9, 3063.5, 3132.6, 3520.8, 4078.8, 5066.2, 5296.5, 5375.5 Da)를 선발하였다.

• Reproductive and Developmental Biology
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• 제35권4호
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• pp.399-405
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• 2011

The number of abandoned dogs is increasing with the worsening of the economy and the rising of feed value. It was becoming a serious social problem because of the disease transmission and destruction of natural ecosystems by abandoned dogs been wild animal. In order to solve these problems, companion dogs necessary to secure its own genetic information and to establish the systematic tracking system. Using multiplex-PCR method with 27 microsatellite marker (MS marker) divided 3 set, various alleles occurring to 6 dog breed (Labrador Retriever, German Shepherd, English Springer Spaniel, Belgian Malinois, Jindo Dog, PoongSan Dog) make use of markers to determine allele frequency and heterozygosity. MS marker FH2834 and FH2790 have only two allele and most were found in 13 alleles at FH3381 and FH3399. Average heterozygosity of MS marker is 0.534 and especially, heterozygosity represented the highest value of 0.765 at FH3381. So, it was recognized appropriate allele frequency for individual identification and paternity diagnosis in companion dogs. Using multiplex-PCR method with MS marker, various alleles occurring to dog breed make use of markers to deter mine individual identification and paternity diagnosis, traits associated biomarkers and breed-specific marker for faster, more accurate and ways to reduce the analysis cost. Based on this result, a scientific basis was established to the existing pedigree data by applying genetics additionally. Animal registration system is expected to be conducted nationwide in future. The method expects to very useful this system.

• 분석과학
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• 제30권6호
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• pp.355-378
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• 2017

신경전달물질(neurochemicals)은 인체 내의 항상성유지와 인지 및 행동기능에 관여하므로 수많은 퇴행성신경질환 진단에 활용할 수 있어 생물학적 시료 내에서 신경화학물질을 프로파일링할 수 있는 분석플랫폼 개발에 대한 관심이 증가하고 있다. 특히, 크로마토그래피 분리법과 결합된 질량분석법 기반의 분석법은 대사경로 내의 신경전달물질을 프로파일링하는 데 널리 사용되어 오고 있다. 하지만 생물학적 시료내 신경전달물질은 극미량으로 존재하며 화학적으로 불안정한 특징이 있어 정교한 시료전처리 과정과 고감도의 기기분석법의 개발이 수반되어야 한다. 따라서 본 총설 논문에서는 소변, 혈액, 뇌척수액과 생체조직과 같은 다양한 생물학적 시료에서 신경전달물질에 대한 질량분석법 기반의 대사체학 접근법의 분석 연구 경향에 대해서 논의할 예정이다. 이 논문은 향후 퇴행성신경질환의 진단, 예후예측과 치료를 가능하게 하는 생체지표물질을 발굴을 위한 분석플랫폼 개발에 기여할 것으로 기대된다.

• Current Research on Agriculture and Life Sciences
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• 제31권1호
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• pp.51-55
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• 2013

예로부터 다양한 방면에서 약용식물로 널리 사용되어 온 감초에서 분리한 dehydroglyasperin C (DGC)는 이전의 연구에서 세포 모델계에서 비교적 높은 항산화 능력과 2상 해독효소계 활성을 유도하는 것이 확인되었으나, 동물 모델계에서 DGC의 항산화능과 2상 해독효소계를 평가하였을 때, 유의적 결과가 관찰되지 않았다. 따라서 DGC 처리시간에 따라 마우스의 장기 및 혈장에 어떠한 영향을 미치는지를 알아보고자 0, 2, 4, 6, 8, 12, 24 시간 동안 DGC를 처리한 후, 장기별 QR 유도활성과 간과 신장에서의 단백질 발현 패턴, 혈장의 항산화능력을 측정하였다. 그 결과 DGC 처리에 의한 QR 유도활성은 위, 대장에서 시간에 따라 변화하는 경향을 보였고, 간, 신장, 소장, 폐에서는 큰 경향성이 나타나지 않았으며, 2상 해독효소의 단백질 발현 패턴은 간에서는 역시 큰 경향성이 나타나지 않았고 위에서는 QR 유도활성과 유사한 경향이 나타남을 확인하였다. 혈장의 DGC 처리 시간에 따른 항산화활성은 시간에 따라 유의적으로 값이 증가한 것을 확인할 수 있었다. 결론적으로 DGC는 처리 시간에 따라 각 장기 및 혈장에 각기 다르게 영향을 미치는 것으로 사료되며, 앞으로도 추가적인 연구를 통하여 DGC의 효능을 보다 구체적으로 검증하는 것이 필요한 것으로 생각된다.

• 대한두경부종양학회지
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• 제33권1호
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• pp.21-29
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• 2017

Methylation of CpG islands in the promoter region of genes acts as a significant mechanism of epigenetic gene silencing in head and neck squamous cell carcinoma (HNSCC). DNA methylation markers are particularly advantageous because DNA methylation is an early event in tumorigenesis, and the epigenetic modification, 5-methylcytosine, is a stable mark. In the present study, we assessed the genome-wide preliminary screening and were to identify novel methylation biomarker candidate in HNSCC. Genome-wide methylation analysis was performed on 10 HNSCC tumors using the Methylated DNA Isolation Assay (MeDIA) CpG island microarray. Validation was done using immunohistochemistry using tissue microarray of 135 independent HNSCC tumors. In addition, in vitro proliferation, migration/invasion assays, RT-PCR and immunoblotting were performed to elucidate molecular regulating mechanisms. Our preliminary validation using CpG microarray data set, immunohisto-chemistry for HNSCC tumor tissues and in vitro functional assays revealed that methylation of the Homeobox B5 (HOXB5) and H6 Family Homeobox 2 (HMX2) could be possible novel methylation biomarkers in HNSCC.

• 생명과학회지
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• 제21권6호
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• pp.893-900
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• 2011

Prostatic acid phosphatase (PAP)는 전립선 암의 진단에 널리 사용되는 표지자로서 1935년 처음으로 동정되었고 인체 전립선에 가장 많이 존재하는 탈 인산화효소이다. PAP는 prostate epithelial cells에서 합성되는 전립선 특이적인 효소로서, 산성 환경에서 효소활성을 띠는 acid phosphatase 그룹에 속한다. PAP는 전립선액에 풍부히 존재하여 수정, 정자부족증, 만성통증의 감소에 관여한다. 그러나 가장 눈에 띄는 기능은 ERK1/2와 MAPK 경로에 관계된 HER-2와 PI3P의 탈 인산화를 유도하여 세포 성장 신호를 억제하고 전립선 암의 억제자로 작용하는 것이다. 최근 PAP DNA 백신을 이용하는 임상시험이 현재 진행 중이고, PAP를 이용한 immunotherapy를 통해 전립선 암을 치료하는 방법이 FDA의 승인을 받아 시행되고 있다. 이러한 PAP의 임상적 중요성에도 불구하고 현재까지 PAP의 분자적 조절기작에 대한 이해는 제한적이라 PAP에 대한 많은 연구가 필요한 실정이다. PAP는 NF-${\kappa}B$, TNF-${\alpha}$, IL-1 및 androgen과 androgen receptor에 의하여 promoter region이 조절된다고 알려졌다. 본 총설에서는 현재까지 밝혀진 PAP 유전자 및 단백질의 특징들과 더불어 전립선 암에서의 PAP의 기능, 발현 조절, 역할들을 종합하였다.

• 대한예방한의학회지
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• 제21권2호
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• pp.1-13
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• 2017

Objectives : This paper serves to explore current trends of systems biology in Traditional Chinese Medicine (TCM) and examine how it may influence the Traditional Korean medicine. Methods : Literature review method was collectively used to classify Introduction to systems biology, diagnosis and syndrome classification of systems biology in TCM perspective, physiotherapy including acupuncture, herbs and formula functions, TCM systems biology, and directions of academic development. Results : The term 'Systems biology' is coined as a combination of systems science and biology. It is a field of study that tries to understand living organism by establishing a theory based on an ideal model that analyzes and predicts the desired output with understanding of interrelationships and dynamics between variables. Systems biology has an integrated and multi-dimensional nature that observes the interaction among the elements constructing the network. The current state of systems biology in TCM is categorized into 4 parts: diagnosis and syndrome, physical therapy, herbs and formulas and academic development of TCM systems biology and its technology. Diagnosis and syndrome field is focusing on developing TCM into personalized medicine by clarifying Kidney yin deficiency patterns and metabolic differences among five patterns of diabetes and analyzing plasma metabolism and biomarkers of coronary heart disease patients. In the field of physical therapy such as acupuncture and moxibustion, researchers discovered the effect of stimulating acupoint ST40 on gene expression and the effects of acupuncture on treating functional dyspepsia and acute ischemic stroke. Herbs and formulas were analyzed with TCM network pharmacology. The therapeutic mechanisms of Si Wu Tang and its series formulas are explained by identifying potential active substances, targets and mechanism of action, including metabolic pathways of amino acid and fatty acid. For the academic development of TCM systems biology and its technology, it is necessary to integrate massive database, integrate pharmacokinetics and pharmacodynamics, as well as systems biology. It is also essential to establish a platform to maximize herbal treatment through accumulation of research data and diseases-specific, or drug-specific network combined with clinical experiences, and identify functions and roles of molecules in herbs and conduct animal-based studies within TCM frame. So far, few literature reviews exist for systems biology in traditional Korean medicine and they merely re-examine known efficacies of simple substances, herbs and formulas. For the future, it is necessary to identify specific mechanisms of working agents and targets to maximize the effects of traditional medicine modalities. Conclusions : Systems biology is widely accepted and studied in TCM and already advanced into a field known as 'TCM systems biology', which calls for the study of incorporating TCM and systems biology. It is time for traditional Korean medicine to acknowledge the importance of systems biology and present scientific basis of traditional medicine and establish the principles of diagnosis, prevention and treatment of diseases. By doing so, traditional Korean medicine would be innovated and further developed into a personalized medicine.

• Toxicological Research
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• 제6권2호
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• pp.205-213
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• 1990

The regulation of neurotoxicants has usually been based upon setting reference doses by dividing a no observed adverse effect level (NOAEL) by uncertainty factors that theoretically account for interspecies and intraspecies extraploation of experimental results in animals to humans. Recently, we have proposed a four-step alternative procedure which provides quantitative estimates of risk as a function of dose. The first step is to establish a mathematical relationship between a biological effect or biomarker and the dose of chemical administered. The second step is to determine the distribution (variability) of individual measurements of biological effects or their biomarkers about the dose response curve. The third step is to define an adverse or abnormal level of a biological effect or biomarker in an untreated population. The fourth and final step is to combine the information from the first three steps to estimate the risk (proportion of individuals exceeding on adverse or abnormal level of a biological effect or biomarker) as a function of dose. The primary purpose of this report is to enhance the certainty of the first step of this procedure by improving our understanding of the relationship between a biomarker and dose of administered chemical. Several factors which need to be considered include: 1) the pharmacokinetics of the parent chemical, 2) the target tissue concentrations of the parent chemical or its bioactivated proximate toxicant, 3) the uptake kinetics of the parent chemical or metabolite into the target cell(s) and/or membrane interactions, and 4) the interaction of the chemical or metabolite with presumed receptor site(s). Because these theoretical factors each contain a saturable step due to definitive amounts of required enzyme, reuptake or receptor site(s), a nonlinear, saturable dose-response curve would be predicted. In order to exemplify this process, effects of the neurotoxicant, methlenedioxymethamphetamine (MDMA), were reviewed and analyzed. Our results and those of others indicate that: 1) peak concentrations of MDMA and metabolites are ochieved in rat brain by 30 min and are negligible by 24 hr, 2) a metabolite of MDMA is probably responsible for its neurotoxic effects, and 3) pretreatment with monoamine uptake blockers prevents MDMA neurotoxicity. When data generated from rats administerde MDMA were plotted as bilolgical effect (decreases in hippocampal serotonin concentrations) versus dose, a saturation curve best described the observed relationship. These results support the hypothesis that at least one saturable step is involved in MDMA neurotoxicity. We conclude that the mathematical relationship between biological effect and dose of MDMA, the first step of our quantitative neurotoxicity risk assessment procedure, should reflect this biological model information generated from the whole of the dose-response curve.