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Yo Ahn Suh,O Min Kwon,So Young Yim,Hee Jae Lee,Sung-Soo Kim 대한생리학회-대한약리학회 2007 The Korean Journal of Physiology & Pharmacology Vol.20 No.3
Kainic acid (KA) causes neurodegeneration, but no consensus has been reached concerning its mechanism. Nitric oxide may be a regulator of the mechanism. We identified differentially expressed genes in the hippocampus of mice treated with kainic acid, together with or without L-NAME, a nonselective nitric oxide synthase inhibitor, using a new differential display PCR method based on annealing control primers. Eight genes were identified, including clathrin light polypeptide, TATA element modulatory factor 1, neurexin III, ND4, ATPase, H+ transporting, V1 subunit E isoform 1, and N-myc downstream regulated gene 2. Although the functions of these genes and their products remain to be determined, their identification provides insight into the molecular mechanism(s) involved in KA-induced neuronal cell death in the hippocampal CA3 area.
Suh, Yo-Ahn,Kwon, O-Min,Yim, So-Young,Lee, Hee-Jae,Kim, Sung-Soo The Korean Society of Pharmacology 2007 The Korean Journal of Physiology & Pharmacology Vol.11 No.4
Kainic acid (KA) causes neurodegeneration, but no consensus has been reached concerning its mechanism. Nitric oxide may be a regulator of the mechanism. We identified differentially expressed genes in the hippocampus of mice treated with kainic acid, together with or without L-NAME, a nonselective nitric oxide synthase inhibitor, using a new differential display PCR method based on annealing control primers. Eight genes were identified, including clathrin light polypeptide, TATA element modulatory factor 1, neurexin III, ND4, ATPase, $H^+$ transporting, V1 subunit E isoform 1, and N-myc downstream regulated gene 2. Although the functions of these genes and their products remain to be determined, their identification provides insight into the molecular mechanism(s) involved in KA-induced neuronal cell death in the hippocampal CA3 area.
Yoo, Yo-Han,Kim, Minjae,Chandran, Anil Kumar Nalini,Hong, Woo-Jong,Ahn, Hye Ryun,Lee, Gang Taik,Kang, Sungju,Suh, Dabin,Kim, Jin-O,Kim, Yeon-Ju,Jung, Ki-Hong MDPI AG 2019 INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES Vol.20 No.23
<P>Plant-growth-promoting bacteria (PGPB) are beneficial microorganisms that can also protect against disease and environmental stress. Silicon (Si) is the second most abundant element in soil, and is known to increase plant growth, grain yield, resistance to biotic stress, and tolerance to abiotic stress. Combined treatment of PGPB and Si has been shown to further enhance plant growth and crop yield. To determine the global effects of the PGPB and Si on rice growth, we compared rice plants treated with Paenibacillus yonginensis DCY84T (DCY84T) and Si with untreated rice. To identify the genes that respond to DCY84T+Si treatment in rice, we performed an RNA-Seq transcriptome analysis by sampling treated and untreated roots on a weekly basis for three weeks. Overall, 576 genes were upregulated, and 394 genes were downregulated in treated roots, using threshold fold-changes of at least 2 (log2) and p-values < 0.05. Gene ontology analysis showed that phenylpropanoids and the L-phenylalanine metabolic process were prominent in the upregulated genes. In a metabolic overview analysis using the MapMan toolkit, pathways involving phenylpropanoids and ethylene were strongly associated with upregulated genes. The functions of seven upregulated genes were identified as being associated with drought stress through a literature search, and a stress experiment confirmed that plants treated with DCY84T+Si exhibited greater drought tolerance than the untreated control plants. Furthermore, the predicted protein-protein interaction network analysis associated with DCY84T+ Si suggests mechanisms underlying growth promotion and stress tolerance.</P>
Hyun Hyesun,Ahn Yo Han,Park Eujin,Choi Hyun Jin,Han Kyoung Hee,Lee Jung Won,Kim Su Young,Yang Eun Mi,Suh Jin-Soon,Shin Jae Il,Cho Min Hyun,Koo Ja Wook,Kim Kee Hyuck,Park Hye Won,Ha Il-Soo,Cheong Hae I 대한소아신장학회 2023 Childhood kidney diseases Vol.27 No.2
Purpose: Angiotensin-converting enzyme inhibitors and angiotensin II receptor blockers (ARBs) are frequently employed to counteract the detrimental effects of proteinuria on glomerular diseases. However, the effects of ARBs remain poorly examined in pediatric patients with immunoglobulin A (IgA) nephropathy. Herein, we evaluated the efficacy and safety of losartan, an ARB, in pediatric IgA nephropathy with proteinuria. Methods: This prospective, single-arm, multicenter study included children with IgA nephropathy exhibiting proteinuria. Changes in proteinuria, blood pressure, and kidney function were prospectively evaluated before and 4 and 24 weeks after losartan administration. The primary endpoint was the difference in proteinuria between baseline and 24 weeks. Results: In total, 29 patients were enrolled and received losartan treatment. The full analysis set included 28 patients who received losartan at least once and had pre- and post-urinary protein to creatinine ratio measurements (n=28). The per-protocol analysis group included 22 patients who completed all scheduled visits without any serious violations during the study period. In both groups, the mean log (urine protein to creatinine ratio) value decreased significantly at 6 months. After 24 weeks, the urinary protein to creatinine ratio decreased by more than 50% in approximately 40% of the patients. The glomerular filtration rate was not significantly altered during the observation period. Conclusions: Losartan decreased proteinuria without decreasing kidney function in patients with IgA nephropathy over 24 weeks. Losartan could be safely employed to reduce proteinuria in this patient population. ClinicalTrials.gov trial registration (NCT0223277)
사람 탯줄로부터 추출된 Type I Collagen의 Telopeptide 제거에 대한 분석
서활,안수진,김요숙,이하규,Suh, Hwal,Ahn, Sue-Jin,Kim, Yo-Sook,Lee, Ha-Gyui 대한의용생체공학회 1996 의공학회지 Vol.17 No.3
Although collagen is still considered to be a poor immunogen, animals can produce antibodies to a number of different sites in the collagen molecule. In type I collagen, three classes of antigenic determinants have been described those are recogrlized as different degrees in different species. These are essentially composed of helical, conformation-dependent antigenic determinants and terminal, nonhelical antigenic determinants, and finally central antigenic determinants exposed only after denaturation of the collagen molecule. To utilize collagen as implantable biomateriall human e61bryonic collagen, ten immunological to body, was purified from human umbilical cords and found to contain [$\alpha$1(I)]$_2$. [$\alpha$2(I). Each step of purification were observed by polarized light microscope and analyzed through SDS-PAGE. The conclusious are follows; 1 . The purified collagen revealed gradual fiber indenties on each step of purification by polarized microscope. 2. The structual changes of extracted collagen as removed telopeptide were confirmed by SDS-PAGE.
유기질과 무기질 복합체를 이용한 체내흡수형 인공골재료에 관한 연구 -세포배양에 의한 생체적합성 평가-
안수진,김요숙,이춘기,서활,Ahn, Sue-Jin,Kim, Yo-Sook,Lee, Choon-Ki,Suh, Hwal 대한의용생체공학회 1995 의공학회지 Vol.16 No.3
체내 매입후 경시적으로 분해되면서 재생골조직에 의해 치환되는 인공골복합체를 제조하고 복합체가 세포활성에 미치는 영향을 조사하였다. 복합체시편을 세포배양액에 넣고 1주일동안 $37^{\circ}C$에서 배양한 다음, 사람자궁경부암유래 HeLa S3세포와 쥐피하 L929세포를 복합체가 용해된 세포배양액에서 5일간 배양하여 세포성장율을 비교하여 세포특성을 조사하였다. 한편 HeLa S3세포를 배양중인 배양액에 ${Na_2}^{51}CrO_4$를 첨가하여 HeLa S3세포에 $^{51}Cr$를 표식한 다음, 용해된 $^{51}Cr$의 양을 $\gamma$-counter를 이용하여 측정하였다. 세포성장정도의 측정에서는 HeLa S3 세포 및 L929 세포 모두가 특이한 세포독성을 발견할 수 없었으며, 복합체가 용해된 세포배양액내의 표식된 HeLa S3 세포로 부터 용해된 $^{51}Cr$량을 측정한 결과, 세포활성을 저해하지 않은 것으로 관찰되었다. A composite material was produced as an artificial bone substitute which is gradually degrAded and replaced by the regenerated natural bones after implantation. To detect the effect of the material on the cell's activity, the composite specimens were placed in MEMs and incubated at $37^{\circ}C$ for one week. Human uterus cervical cancer origin HeLa 3 cells and mouse subcutaneous origin L929 cells were cul- tured in the specimen dissolved MEMs for 5 days to investigate cytotoxicity via cell growth rates. ${Na_2}^{51}CrO_4$ solution was added to the media, to label the HeLa 53 cells, and the released amount of $^{51}Cr$ was measured by a $\gamma$-counter. On the cell growth investigation, no significant cytotoxic phenomena were revealed in both HeLa S3 and L929 cell cultures. On the released 51CR from the incubated HeLa 53 cells, no significant cell degeneration was observed from the composite embedded MEMs.
Type I Atelocollagen의 가교형성비 분석
안수진,김요숙,서활,Ahn, Soo-Jin,Kim, Yo-Sook,Suh, Hwal 대한의용생체공학회 1996 의공학회지 Vol.17 No.4
To utilize collagen as an implantable biomateriall the mcct widely used bovine skin origin Type I collagen was investigated Pepsin treated, Type I atelocollagen was extracted and crosslinked by the ultraviolet(W) ray with wavelength of 254nm or by various concentrations of glutaraldehyde to produce collagen membranes. The crosslink rates of the specimens were observed by a polarized light microscope, a scanning electron microscope, and a Fourier transform infrared (FT-lR) spectrometer. The followings are concluded 1. The collagen membranes produced by both 2.5% glutaraldehyde solution and 254nm UV ray irra- diation demonstrated similar morphologies on polarized light microscopic and scanning electron microscopic views. 2. The chemical structures of the crosslinked membranes by glutaraldehyde over 2.5% in concentrations revealed similar intensities to that of the UV ray irradiated one in FT-lR investigation. 3. To obtain optimal croulink in bovine stalin origin Type I atelocollagen, 2.5% glutaraldehyde solution or UV ray irradiation with 254nm wavelength is acceptable.
Gorham-Stout Syndrome with Focal Segmental Glomerulosclerosis: A Case Report
Kim, Ji Hyun,Kim, You Sun,Lim, Seon Hee,Ahn, Yo Han,Ko, Jung-Min,Suh, Dong In,Lee, Kyoung Bun,Moon, Kyung Chul,Ha, Il-Soo,Cheong, Hae Il,Kang, Hee Gyung Korean Society of Pediatric Nephrology 2020 Childhood kidney diseases Vol.24 No.2
Gorham-Stout syndrome is a rare bone disorder characterized by progressive massive osteolysis and proliferation of vascular and lymphatic vessels. A 15-year-old boy was initially diagnosed with Gorham-Stout at the age of 8 years based on clinical and radiological findings. Following diagnosis, he was treated with pamidronate, interferon alfa, propranolol, oral corticosteroids, and sirolimus. He developed proteinuria at the age of 15 and progressed into the nephrotic range 2 years later. A renal biopsy revealed focal segmental glomerulosclerosis, not otherwise specified variant. The sequential increase in proteinuria associated with medications suggested that the focal segmental glomerulosclerosis may be caused by pamidronate and sirolimus, but cannot completely rule out the possibility of kidney involvement of GSS itself.
Gorham-Stout Syndrome with Focal Segmental Glomerulosclerosis: A Case Report
Ji Hyun Kim,You Sun Kim,Seon Hee Lim,Yo Han Ahn,Jung-Min Ko,Dong In Suh,Kyoung Bun Lee,Kyung Chul Moon,Il-Soo Ha,Hae Il Cheong,Hee Gyung Kang 대한소아신장학회 2020 Childhood kidney diseases Vol.24 No.2
Gorham-Stout syndrome is a rare bone disorder characterized by progressive massive osteolysis and proliferation of vascular and lymphatic vessels. A 15-yearold boy was initially diagnosed with Gorham-Stout at the age of 8 years based on clinical and radiological findings. Following diagnosis, he was treated with pamidronate, interferon alfa, propranolol, oral corticosteroids, and sirolimus. He developed proteinuria at the age of 15 and progressed into the nephrotic range 2 years later. A renal biopsy revealed focal segmental glomerulosclerosis, not otherwise specified variant. The sequential increase in proteinuria associated with medications suggested that the focal segmental glomerulosclerosis may be caused by pamidronate and sirolimus, but cannot completely rule out the possibility of kidney involvement of GSS itself.