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Kim, Hyungrok;Choi, Yongwoo;Kwon, Osung;Chung, Hyun;Park, Joonsoo;Park, Kyung-Duck
- Korean journal of dermatology
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- v.56 no.9
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- pp.561-562
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- 2018
KSCI

Yoon, Junghwan;Kye, Min-Surk;Lee, Woong-Woo;Kang, Kyusik;Park, Jong-Moo;Kim, Byung-Kun;Kwon, Ohyun;Lee, Jung-Ju
- Journal of the Korean neurological association
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- v.36 no.4
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- pp.396-398
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- 2018
https://doi.org/10.17340/jkna.2018.4.30 인용

Han, Tae-Young;Na, Chan Ho;Lee, Ji Hyun;Kim, Hye One;Park, Chang Ook;Seo, Young Joon;Son, Sang Wook;Shin, Min Kyung;Ahn, Ji Young;Lee, Yang Won;Jang, Yong Hyun;Park, Young Lip;Lew, Bark Lynn
- Korean journal of dermatology
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- v.56 no.10
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- pp.581-593
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- 2018
Atopic dermatitis (AD) is a common, chronic, relapsing, inflammatory skin disease that affects both children and adults. AD is the cause of considerable morbidity including severe pruritus and impaired quality of life. Treatments for active disease include avoidance of triggering factors, barrier repair, topical medications including topical corticosteroids (TCs) and topical calcineurin inhibitors (TCIs), phototherapy, antibacterial agents, and systemic immunosuppressants including cyclosporine. Until recently, the only Food and Drug Administration (FDA)-approved systemic treatment options for patients with moderate-to-severe AD were steroids and cyclosporine. Systemic steroids are not recommended by current guidelines and are commonly associated with disease rebound. Instead, clinicians choose from several off-label immunosuppressants. In 2018, the Korean FDA approved dupilumab for adults with moderate-to-severe AD whose disease is not adequately controlled with topical therapies. The implementation of treatment guidelines for AD is challenging. Herein, we review the several treatment modalities for AD and recommend a treatment algorithm.
KSCI

Kang, Jongsoo;Kim, Min Ok;Yi, Jeong Jin;Park, Min Won;Kim, Chang Hun;Kim, Young-Soo;Park, Kee Hong;Kang, Hee-Young;Choi, Nack-Cheon;Kwon, Oh-Young;Kim, Soo-Kyoung
- Journal of the Korean neurological association
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- v.36 no.4
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- pp.337-340
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- 2018
Human immunodeficiency virus (HIV) infection can result in ischemic stroke via several mechanisms, including opportunistic infection, vasculopathy, cardioembolism, and coagulopathy. HIV-vasculopathy is related to endothelial dysfunction, stenosis and aneurysm formation, infectious vasculitis, dissection and accelerated atherosclerosis during highly active antiretroviral therapy (HAART). We represent a case of HIV infection manifested as an acute ischemic stroke attack. After 4 months during HAART, our patient experienced a recurrent ischemic stroke with progression of middle cerebral artery stenosis.
https://doi.org/10.17340/jkna.2018.4.13 인용

Yi, Jae-Hong;Shin, Yu-Yong;Noh, Kyung-Chul;Chung, Sung Eun;Lee, Dokyung;Lee, Yeon-Ah;Ahn, Tae-Beom
- Journal of the Korean neurological association
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- v.35 no.4
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- pp.244-246
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- 2017
https://doi.org/10.17340/jkna.2017.4.14 인용

Song, Jae Hwang;Kang, Chan;Kim, Sang Bum;Heo, Youn Moo;Won, You Gun;Jung, Sang Jin;Chung, Hyung Jin
- Journal of Korean Foot and Ankle Society
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- v.22 no.4
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- pp.184-184
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- 2018
https://doi.org/10.14193/jkfas.2018.22.4.184 인용 PDF KSCI

오양효;김영부;김미경;김민정;윤소겸
- Journal of Life Science
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- v.4 no.2
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- pp.60-63
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- 1994
Protein A는 Jensen법에 의하여 Staphylococcus aureus Cowan type 1 (SCI)주의 가열균 체에서 추출한 단백으로서 최근에는 lysostaphin-chromatography 방법으로 순수분리할 수 있는 natural protein이다. Protein A를 다량 함유한 SCI은 혈청중의 IgG를 흡착하므로 혈청 중에 IgG를 제거할 목적으로 사용할 수 있다. 본고에서는 protein A가 면양적혈구로 면역한 가토혈청의 적혈구 응집소가 및 용혈소가에 미치는 영향을 기술하였다.
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