1.Micronuclei in Peripheral Blood Lymphocytes of Chromate Workers.
Jung Ho RAH ; Young Whan KIM ; Jae Wook CHOI ; Hae Joon KIM
Korean Journal of Occupational and Environmental Medicine 1999;11(3):393-406
No abstract available.
Lymphocytes*
2.Determination of % PRA and identification of HLA antibody using home-made lymphocytes panel.
Korean Journal of Blood Transfusion 1992;3(1):71-77
No abstract available.
Lymphocytes*
3.Differentiation of B cells.
Journal of the Korean Pediatric Society 1993;36(7):901-905
No abstract available.
B-Lymphocytes*
4.T-cell mediated immunity in pulmonary and extrapulmonary tuberculos- is.
Dong Chull CHOI ; Tae Sun SHIM ; Sang Hoon CHO ; Ki Ho JUNG ; In Gyu HYUN ; Chul Gyu YOO ; Young Whan KIM ; Young Soo SHIM ; Keun Youl KIM ; Yong Cho HAN
Tuberculosis and Respiratory Diseases 1992;39(1):62-72
No abstract available.
T-Lymphocytes*
5.Study on application of hyperchem program for calculating the kinetics and optimal procedure of staining non--specific esterase of human lymphocyte
Journal of Medical and Pharmaceutical Information 2001;(6):18-24
By using the hyperchem program, authors calculated quantitatively the change about the charge and stereo structure of molecules along various stages of the reaction of non-specific esterase (ANAE); Simultaneously, the changes of torsion, angle, energy, bond length were showed. That is evident to prove correlatively the kinetic mechanism of the electrophin substitute reaction. From the above calculations, the factors that affect to the optimum process for a highest effect of ANAE cytochemistry can be deduced
Lymphocytes
;
Esterases
6.Eosiniphilic Gastroenteritis in Childhood and Competitive RT-PCR, In vitro Lymphocyte Prokiferation Response to Food Antigens.
Journal of the Korean Pediatric Society 1996;39(11):1498-1503
No abstract available.
Gastroenteritis*
;
Lymphocytes*
7.In reply: Tumor-associated lymphocytes expanded ex vivo from malignant ascites.
Journal of Gynecologic Oncology 2010;21(2):133-133
No abstract available.
Ascites
;
Lymphocytes
9.Influence of radiation therapy on T lymphocyte and subsets in peripheral blood of various cancer patients.
Chang Geun JEONG ; Woo Song HA ; Soon Tae PARK ; Soon Chan HONG ; Ho Seong HAN ; Sang Beom KIM ; Kyu Young CHAE ; Ok Jae LEE
Journal of the Korean Surgical Society 1993;45(5):765-774
No abstract available.
Humans
;
Lymphocytes*
10.Association of Neutrophil-to-Lymphocyte Ratio (NLR) and Platelet-to-Lymphocyte Ratio (PLR) to disease activity in Filipino lupus patients
Francis Martin T CUENCO ; Sandra V NAVARRA
Journal of Medicine University of Santo Tomas 2020;4(1):455-461
Background:
Systemic lupus erythematosus (SLE)
is a chronic, multisystem, autoimmune disease characterized by autoantibody production, immune
complex deposition and excessive pro-infl ammatory
cytokine production due to an aberrant and dysfunctional immune system. Disease activity markers for
SLE are helpful in the management and prognostication of the disease. The neutrophil-to-lymphocyte ratio (NLR) and platelet-to-lymphocyte ratio (PLR) have
been studied as a novel infl ammatory marker and
prognostic markers for cardiovascular diseases, infl ammatory disorders and malignancies.
Objective:
The aim of the study is to investigate
the association of NLR and PLR to disease activity of
Filipino patients with SLE.
Methods:
This is a cross-sectional study done
through a retrospective chart review of 135 Filipino
SLE patients divided into two groups. Group 1
(SLEDAI-2K score of <3) had 64 patients who were in
low disease activity/remission and group 2 (SLEDAI2K score of ≥3) had 71 patients who were in active
disease. Clinical characteristics and disease activity
parameters (C3, anti-dsDNA, ESR) and NLR and PLR were compared in the two groups. Correlations of
NLR and PLR with established clinical and laboratory disease activity markers of SLE (C3, anti-dsDNA,
SLEDAI-2K scores) were analyzed.
Results:
The group 2 or those with active disease
had signifi cantly higher NLR (2.947 ± 1.756 vs.
1.868 ± 0.832, p-value of <0.001) and PLR (205.9
± 122.2 vs. 140.2 ± 53.0, p-value of <0.001) levels compared to group 1. NLR and PLR values were
also signifi cantly higher in patients with lupus nephritis. NLR was positively correlated with anti-dsDNA (r = +0.490, p-value of <0.001) and SLEDAI-2K
scores (r = +0.496, p-value of <0.001). NLR was
negatively correlated with C3 (r = -0.336, p-value
of <0.001). PLR was also positively correlated with
anti-dsDNA (r = +0.301, p-value of <0.001) and
SLEDAI-2K scores (r = +0.369, p-value <0.001). PLR
was also negatively correlated with C3 levels (r =
-0.215, p-value 0.012). Using the ROC curve analysis, the cut-off values in predicting active disease in
SLE were 1.968 (sensitivity 77.5%, specifi city 75%)
for NLR and 144.53 (sensitivity 63.4%, specifi city
60%) for PLR. The cut-off values in predicting lupus
nephritis were 2.121 (sensitivity 73.1%, specifi city
60%) for NLR and 167.0 (sensitivity 65.4%, specifi city 68%) for PLR.
Conclusions
NLR and PLR were signifi cantly higher among Filipino SLE patients with active disease
including lupus nephritis refl ecting active infl ammation. NLR and PLR correlated well with established disease activity markers for SLE namely C3, anti-dsDNA, and SLEDAI-2K scores. NLR and PLR could
be a useful and convenient disease activity marker
for SLE patients.
Neutrophils
;
Lymphocytes
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