Yuri Kim
Yonsei University
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Publication
Featured researches published by Yuri Kim.
Biology of Blood and Marrow Transplantation | 2012
Ji Eun Jang; Shin Young Hyun; Yun Deok Kim; Sul Hee Yoon; Doh Yu Hwang; Soo Jeong Kim; Yuri Kim; Jin Seok Kim; June Won Cheong; Yoo Hong Min
Cytomegalovirus (CMV) disease is a major cause of infectious complications in allogeneic hematopoietic stem cell transplantation (allo-HSCT). Although patients undergoing allo-HSCT receive prophylactic and preemptive treatment for CMV, a subset of patients experience clinically significant CMV disease. This study investigated the risk factors for progression from CMV viremia to CMV disease during or after preemptive therapy in patients undergoing allo-HSCT. Between January 2006 and August 2010, 43 patients received preemptive therapy for CMV viremia after allo-HSCT. These patients experienced 74 episodes of CMV viremia. Nine of the patients (21%) and 12 of the episodes (16%) progressed to CMV disease. Univariate analysis identified several risk factors for progression to CMV disease, including high initial viral load (Pxa0=xa0.020), leukopenia (P = .012), and neutropenia (P = .033) at the time of detection of CMV viremia. On multivariate analysis, leukopenia remained an independent predictor (hazard ratio, 4.347; P = .045). The rate of failure to clear CMV viremia after 1 cycle of preemptive therapy was higher in the leukopenia group than in the non-leukopenia group (60.0% versus 16.9%; P = .002). This indicates that leukopenia initiallyxa0documented with CMV viremia is related to lower viral response to preemptive therapy and is a notable risk factor for progression from CMV viremia to CMV disease.
Cell Transplantation | 2017
Ja Kyung Kim; Soo Jeong Kim; Yuri Kim; Yong Eun Chung; Young Nyun Park; Hyun Ok Kim; Jin Seok Kim; Mi-Suk Park; Isao Sakaida; Do Young Kim; Jung Il Lee; Sang Hoon Ahn; Kwan Sik Lee; Kwang Hyub Han
Although several human clinical trials using various bone marrow-derived cell types for cirrhotic or decompensated patients have reported a short-term benefit, long-term follow-up data are limited. We analyzed the long-term clinical outcomes of autologous bone marrow cell infusion (ABMI) for decompensated liver cirrhosis (LC). Patients enrolled in a pilot single-armed ABMI study were followed up more than 5 years. Bone marrow-derived mononuclear cells (BM-MNCs) from decompensated LC were harvested and after processing were infused into a peripheral vein. The laboratory test results and long-term clinical course including liver transplantation (LT), development of cancer, cause of death, and survival after ABMI were analyzed. Nineteen patients were followed up for a median of 66 months after ABMI. Liver function, including serum levels of albumin and Child–Pugh (CP) score, was improved at the 1-year follow-up. Liver volume was significantly greater, cirrhosis was sustained, and collagen content was decreased at the 6-month follow-up. Five years after ABMI, five patients (26.3%) maintained CP class A without LT or death, and five patients (26.3%) had undergone elective LT. Hepatocellular carcinoma (HCC) occurred in five patients (26.3%), and lymphoma and colon cancer occurred in one patient each. Three patients (15.8%) were lost to follow-up at months 22, 31, and 33, respectively, but maintained CP class A until their last follow-up. Five patients expired due to infection. While improved liver function was maintained in some patients for more than 5 years after ABMI, other patients developed HCC. Further studies of long-term follow-up cohorts after cell therapy for LC are warranted.
Biology of Blood and Marrow Transplantation | 2012
Ji Eun Jang; Shin Young Hyun; Yun Deok Kim; Sul Hee Yoon; Doh Yu Hwang; Soo Jeong Kim; Yuri Kim; Jinseok Kim; June-Won Cheong; Yoo Hong Min
Cytomegalovirus (CMV) disease is a major cause of infectious complications in allogeneic hematopoietic stem cell transplantation (allo-HSCT). Although patients undergoing allo-HSCT receive prophylactic and preemptive treatment for CMV, a subset of patients experience clinically significant CMV disease. This study investigated the risk factors for progression from CMV viremia to CMV disease during or after preemptive therapy in patients undergoing allo-HSCT. Between January 2006 and August 2010, 43 patients received preemptive therapy for CMV viremia after allo-HSCT. These patients experienced 74 episodes of CMV viremia. Nine of the patients (21%) and 12 of the episodes (16%) progressed to CMV disease. Univariate analysis identified several risk factors for progression to CMV disease, including high initial viral load (Pxa0=xa0.020), leukopenia (P = .012), and neutropenia (P = .033) at the time of detection of CMV viremia. On multivariate analysis, leukopenia remained an independent predictor (hazard ratio, 4.347; P = .045). The rate of failure to clear CMV viremia after 1 cycle of preemptive therapy was higher in the leukopenia group than in the non-leukopenia group (60.0% versus 16.9%; P = .002). This indicates that leukopenia initiallyxa0documented with CMV viremia is related to lower viral response to preemptive therapy and is a notable risk factor for progression from CMV viremia to CMV disease.
Yonsei Medical Journal | 2007
Jin Seok Kim; Jee Sook Hahn; Sun Young Park; Yuri Kim; In Hae Park; Chun Kyon Lee; June Won Cheong; Seung Tae Lee; Yoo Hong Min
Blood | 2006
Jin Seok Kim; Soo-Jeong Kim; Hye Won Lee; Sul Hee Yoon; In-Hae Park; Yuri Kim; June-Won Cheong; Yoo-Hong Min
Blood | 2011
Yoo-Hong Min; Sulhee Yoon; Doh Yu Hwang; Yundeok Kim; Yeo-Kyeoung Kim; Yuri Kim; Jae Yong Cho; Jin Seok Kim; Soo Jeong Kim; June-Won Cheong; Hyeoung Joon Kim
Blood | 2007
June-Won Cheong; Ju In Eom Eom; Hye Won Lee; In-Hae Park; Yuri Kim; Jinseok Kim; Yoo-Hong Min
Blood | 2006
Soo-Jeong Kim; Hye Won Lee; Sul Hee Yoon; In-Hae Park; Yuri Kim; Jin Seok Kim; June-Won Cheong; Yoo-Hong Min
Blood | 2005
In Hae Park; June-Won Cheong; Jee Young Lee; Jinseok Kim; Hyun Ju Chun; Yuri Kim; Sun Young Park; Jin Koo Lee; Yoo-Hong Min
Blood | 2005
Sun Young Park; Jinseok Kim; Yuri Kim; In Hae Park; Hyun Ju Chun; June-Won Cheong; Yoo-Hong Min