• 대한바이러스학회지
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• 제27권1호
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• pp.97-104
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• 1997

For 16 years after the finding of HIV as an agent of AIDS in 1981, HIV therapeutic drugs of reverse transcriptase inhibitors (AZT, ddI, ddC, d4T) and protease inhibitors have been developed. Recent studies also were focused on a combination therapy by using HIV therapeutic drugs or natural compounds. Korean red ginseng (KRG) of natural compounds has been well known as a good reinforcement agent in Asia. The percentage of CD3+CD4+ T cell in nine HIV-infected patients without KRG treatment averaged 17.8% on baseline and decreased 15.8% after 6 months, whereas the percentage of the cell in fifteen HIV-infected patients with KRG treatment averaged 15.3% on baseline and increased up to 18.9% after the same period. The average percentage of CD3+CD8+ T cell of KRG-nontreated and KRG-treated HIV patients increased after 6 months 47.8% to 50.7% and 44.7% to 51.4%, respectively; and the average percentage of B and NK cell in the KRG-nontreated and KRG-treated HIV patients decreased 9.4% to 7.9% and 13.0% to 9.7%, 8.9% to 8.5% and 16.2% to 11.6%, respectively. KRG, therefore, didn't have any effects on the CD3+CD8+ T cell, B cell, and NK cell. However, it seems that KRG has a potential activity for stimulatiing the CD3+CD4+ T cell and some inhibition on destroying of this cell with no significance.

• Toxicological Research
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• 제11권1호
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• pp.15-21
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• 1995

Several populations of lymphocytes possess receptors for autonomic neurotransmitter, which make lymphocytes susceptible to autonomic stimulation. This study was to evaluate the functional alternation of effector cells of the immune system. Female Balb/C mice, 15-20 g, were injected with MA subcutaneously under various conditions. Mixed lymphocyte reaction (MLR) showed certain T cell subsets were affected by MA. The level of interleukin-2 (IL-2) production was inhibited due to a defect in expression of the IL-2 receptor. In mice injected with 20 mg MA/kg, 1 day before assay, phagocytosis of peritoneal macrophages showed $14.07\pm3%$, which was similar degree to 5 mg MA/kg treatment for 4 consecutive days. Phagocytosis was almost recovered to that of control after 4 day in 20 mg/kg injected mice. Maximum inhibition of plaque forming cell (PFC) occurred when MA was given early, indicating the inductive time point of antibody production was affected. The cortisol level increased in the MA treated group (0.05, 0.20, and $0.08{\mu}g$/dl for control, low, and high dose-MA treated mice, respectively). Based on these results, MA has general suppression effects on the immune systems by functional alteration of effector cells. Considering the increment of serum cortisol levels, MA partially impacts the neuroendocrine system to lead to failure of immune response.

• Asian Pacific Journal of Cancer Prevention
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• 제13권11호
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• pp.5909-5913
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• 2012

Aims: We aimed to analyze the phenotype of tumor-infiltrating lymphocytes (TILs) and non-tumor infiltrating lymphocytes (NILs) in HCC and non-tumor tissues, and evaluate relationships between changes in these cells and the prognosis of HCC. Methods: Lymphocytes were isolated from HCC and corresponding non-tumor tissues and tested by flow cytometry. For comparison, clinical parameters were analyzed. Results: Compared with the non-tumor tissue, tumor tissue had a lower intensity of NK, NKT andCD8+T cell infiltration. TILs had higher intensity of CD4+CD25+Foxp3+regulatory T cell (Treg cells) infiltration compared with that in NILs. The prevalence of Treg cells was associated with fewer CD8 + T lymphocytes in the HCC immune microenvironment. The frequencies of NK cells and CD8+T cells in TILs of HCC patients with metastasis less than 12 months were lower than those without metastasis. However, the frequency of Treg cells was higher than those without metastasis. Conclusion: These results suggest that the frequencies of CD8+T, NK and NKT cells as well as Treg cells in the tumor tissue of HCC are significantly associated with patient survival, and could be applied as predictive indicators for HCC prognosis.

• Parasites, Hosts and Diseases
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• 제31권3호
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• pp.249-258
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• 1993

원발성 아메바성 수막뇌염을 야기하는 Naegleria fowleri를 사망율에 따라 $1{\;}{\times}{\;}10^4$개 아메바 영양형 접종군과. $1{\;}{\times}{\;}10^5$개 아메바 영양형 접종군으로 나누어 비장세포를 비특이 mitogen인 Phytohemagglutinin(PHA)과 특이항원인 N. fowleri Iysates로 자극하여 T 세포의 interleukin-2 생성정도를 측정하고 T 림프구의 아형 및 아세포화정도를 측정한 결과 N.fowleri 아메바 영양형 $1{\;}{\times}{\;}10^5$개 접종군에서의 마우스 사망율은 72.2%였으며 $1{\;}{\times}{\;}10^4$개 접종군에서의 마우스 사망율은 14.3%였다. 또한 IL릭 생성정도를 접종후 7, 14, 24일째 측정한 결과. 접종 후 14일째에는 두 실험군 모두에서 대조군과 비교하여 IL닉의 생성이 유의하게 감소하였으며 접종 후 24일째에는 두 실험군 모두에서 접종 후 14일째 보다는 증가하였으나 대조군과 비교하여 유의하게 억제되었다 비장세포내 T 림프구 아형의 변동은 전체 비장 림프구에 대한 $Thy-1.2^{+}{\;}T.{\;}L3T4^{+}{\;}T,{\;}Ly^{2+}{\;}T$ 세포는 N.fowleri아메바 영양형 $1{\;}{\times}{\;}10^5$개 접종군에서 접종 후 7일째 대조군과 비교하여 유의하게 증가하였고 접종 후 14일째와 24일째에는 대조군과 비교하여 유의한 차이가 없었다. 아메바 영양형 $1{\;}{\times}{\;}10^4$개를 접종시킨 실험군은 경과 일수에 관계없이 대조군과 비교하여 유의한 차이가 없었다. 비장세포내 T 세포의 DNA의 분획을 관찰한 결과 두 실험군 모두에서 접종 후 7일째에 S phase 분획이 가장 높이 증가하였으며 접종 후 14일과 24일째에도 대조군에 비하여는 유의하게 증가하여 있었다. 이상의 결과를 종합하여 볼 때, N.fowleri를 사망율을 기준으로 접종량을 달리하여 아메바 영양형 $1{\;}{\times}{\;}10^4$개 접종군과 $1{\;}{\times}{\;}10^5$개 접종군으로 나누어 접종하였을 때, 접종 후 7일을 전후하여 IL-2를 매개로 활성화되는 세포매개성 면역이 N.fowleri감염의 방어기작으로 작용하는 것으로 생각되며 아메바 접종 후 14일째에는 치명적인 수막뇌염으로 진행되어 비장세포의 IL-2의 생성능력이 매우 억제된 것으로 생각된다. 또한 IL-2 생성능력과 T 세포의 아세포화의 증가 및 T세포 아령의 수의 변동과는 잘 일치되지 않는 것으로 나타났다.

• Clinical and Experimental Pediatrics
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• 제51권5호
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• pp.492-499
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• 2008

목 적 : H. pylori의 감염은 세균의 병독 인자, 숙주 인자, 환경 인자가 복합적으로 작용하여 다양한 위장관 병변을 일으킨다. H. pylori의 병리 기전으로 지금까지는 주로 세균의 병독성에 초점을 맞추었으나 최근에는 숙주의 위점막 면역반응이 주목을 받고 있다. 소아는 술, 담배, 약물과 같은 환경 인자의 영향이 적어 연구에 적합한 대상이며 감염 초기를 반영한다는 측면에서 중요한 의의가 있음에도 불구하고 소아에서 위점막 면역반응에 관한 연구가 거의 없다. 이에 H. pylori 감염 소아에서 위점막 림프구를 분석하여 소아에서 H. pylori 감염으로 인한 국소 면역반응의 특징을 알아보고자 하였다. 방 법 : H. pylori 양성 소화궤양군 10명, H. pylori 양성 위염군 15명, H. pylori 음성 대조군 20명에서 얻은 위전정부 생검조직에서 hematoxylin-eosin 염색과 modified Giemsa 염색을 시행하여 개정된 시드니 체계에 따라 위염의 정도를 점수화하였다. 위점막에서 림프구 면역표현형을 알기 위해 CD3, CD4, CD8 T세포와 CD20 B세포에 대한 면역조직화학염색을 시행하였으며 점막 고유층에서는 400배 고배율 현미경 하에서 $0.0625m^2$ 당 양성 림프구 수를 기록하였고, 상피세포 내에서는 100개 상피세포 당 양성 림프구 수를 기록하였다. 결 과 : 림프구 침윤은 점막 고유층에서 상피세포 내보다 확연히 많았다. 점막 고유층에서 H. pylori 양성군에서 대조군에 비해 CD3, CD4, CD8 T세포와 CD20 B세포가 유의하게 증가하였고(P<0.01) H. pylori 양성 소화궤양군은 위염군과 달리 대조군에 비해 CD8 T세포가 유의하게 증가하였다(P<0.01). 한편, 상피세포 내에서는 H. pylori 양성 소화궤양군과 위염군 모두 대조군에 비해 CD4 T세포가 유의하게 증가하였다(P<0.01). H. pylori의 밀도, 다핵형 중성구의 활동성, 만성 염증 정도와 림프구 수는 점막 고유층에서 상피세포 내보다 더 밀접한 상관관계가 있었다. 결 론: H. pylori에 감염된 소아의 국소 면역반응은 주로 위점막 고유층에서 일어나며 T세포와 B세포가 함께 관여하였다. H. pylori 양성 소화궤양군에서 점막 고유층의 CD8 T세포가 유의하게 증가하여 임상질환과 점막면역의 연관성을 추정할 수 있었다. 향후 H. pylori 감염에서 국소 면역반응으로 야기되는 점막 손상, 연령과 인종에 따른 차이, 임상질환과의 연관성 등에 대하여 더 많은 연구가 이루어져야 할 것이다.

• Journal of Ginseng Research
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• 제44권4호
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• pp.619-626
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• 2020

Background: The effects of diol-ginsenoside fraction (Diol-GF) and triol-ginsenoside fraction (Triol-GF) from Korean Red Ginseng on the development of type 1 diabetes (T1D) were examined in diabetes-prone biobreeding (DP-BB) rats that spontaneously develop T1D through an autoimmune process. Methods: DP-BB female rats were treated with Diol-GF or Triol-GF daily from the age of 3-4 weeks up to 11-12 weeks (1 mg/g body weight). Results: Diol-GF delayed the onset, and reduced the incidence, of T1D. Islets of Diol-GF-treated DP-BB rats showed significantly lower insulitis and preserved higher plasma and pancreatic insulin levels. Diol-GF failed to change the proportion of lymphocyte subsets such as T cells, natural killer cells, and macrophages in the spleen and blood. Diol-GF had no effect on the ability of DP-BB rat splenocytes to induce diabetes in recipients. Diol-GF and diol-ginsenoside Rb1 significantly decreased tumor necrosis factor α production, whereas diol-ginsenosides Rb1 and Rd decreased interleukin 1β production in RAW264.7 cells. Furthermore, mixed cytokine- and chemical-induced β-cell cytotoxicity was greatly inhibited by Diol-GF and diol-ginsenosides Rc and Rd in RIN5mF cells. However, nitric oxide production in RAW264.7 cells was unaffected by diol-ginsenosides. Conclusion: Diol-GF, but not Triol-GF, significantly delayed the development of insulitis and T1D in DP-BB rats. The antidiabetogenic action of Diol-GF may result from the decrease in cytokine production and increase in β-cell resistance to cytokine/free radical-induced cytotoxicity.

• 동의생리병리학회지
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• 제20권6호
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• pp.1636-1648
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• 2006

There are detailed descriptions of the clinical experiences and prescriptions of asthma in traditional Korean medicine. Zedoariae rhizoma is one of the Korean herbal medicines used to treat bronchial asthma and allergic rhinitis for centuries. However, the therapeutic mechanisms of this medication are still far from clear, In this study, a house-dust-mite (Dermatophagoides pteronyssinus [Der p])-sensitized murine model of asthma was used to evaluate the immunomodulatory effect of Zedoariae rhizoma on the allergen-induced airway inflammation in asthma. Three different protocols were designed to evaluate the treatment and/or long-term prophylacitic effect of Zedoariae rhizoma in Der p-sensitized mice. Cellular infiltration and T-cell subsets in the bronchoalveolar lavage fluid (BALF)of allergen-challenged mice were analyzed. Intrapulmonary lymphocytes were also isolated to evaluate their response to allergen stimulation. When Zedoariae rhizoma was administered to the sensitized mice before AC (groups A and C), it suppressed airway inflammation by decreasing the number of total cells and eosinophil infiltration in the BALF, and downregulated the allergen- or mitogen-induced intrapulmonary lymphocyte response of sensitized mice as compared to those of controls. This immunomodulatory effect of Zedoariae rhizoma may be exerted through the regulation of T-cell subsets by elevation or activation of the CD8+ and double-negative T-cell population in the lung. However, the administration of Zedoariae rhizoma to sensitized mice 24 h after AC (group B) did not have the same inhibitory effect on the airway inflammation as Zedoariae rhizoma given before AC. Thus, the administration of Zedoariae rhizoma before AC has the immunomodulatory effect of reducing bronchial inflammation in the allergen-sensitized mice. On the other hand, to determine the potentiality of prophylactic and/or therapeutic approaches using a traditional herbal medicine, Zedoariae rhizoma, for the control of allergic disease, we examined the effects of oral administration of Zedoariae rhizoma on a murine model of asthma allergic responses. When oral administration of Zedoariae rhizoma was begun at the induction phase immediately after OVA sensitization, eosinophilia and Th2-type cytokine production in the airway were reduced in OVA-sensitized mice following OVA inhalation. These results suggest that the oral administration of Zedoariae rhizoma dichotomously modulates allergic inflammation in murine model for asthma, thus offering a different approach for the treatment of allergic disorders.

• 한국식품영양과학회지
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• 제42권12호
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• pp.1930-1939
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• 2013

본 연구에서는 천연 식품으로부터 면역증진능을 갖는 식품 소재를 검색하기 위한 연구의 일환으로 골대사 약화 상태의 마우스에게 청국장 배합 사료를 투여했을 때 카제인 배합사료에 비하여 가질 수 있는 세포 매개성 면역능의 증강 효과를 규명하기 위한 목적으로 실시되었다. 제 1단계로서 난소적출군은 저칼슘 식이, Sham군은 AIN-76 식이를 6주간 공급한 후, 각 군을 청국장 배합 사료군 혹은 카제인 배합사료군으로 나누어 8주간 제 2단계의 식이를 공급하였다. 면역 지표로는 비장세포 증식능, 혈중 T 림프구 아형수와 혈중 사이토카인(IL-2, IL-4, IL-6, IL-10, IFN-${\gamma}$, TNF-${\alpha}$)의 분비량을 측정하였다. 그 결과 난소적출군에서 청국장배합 사료군의 비장 세포 증식능이 카제인 배합 사료군보다 유의적으로 높았으며, 혈중 T 림프구 아형 비율인 CD4/CD8의 비율도 청국장 배합 사료군에서 더 높았다. 혈중 사이토카인 분비량을 측정한 결과 난소적출군에서 청국장 배합 사료 투여군의 IL-6와 TNF-${\alpha}$ 분비량이 카제인 배합 사료 투여군에 비해 유의적으로 낮았다. 난소적출 마우스의 면역능에 청국장 배합 사료가 미치는 영향으로 카제인 배합사료에 비하여 비장 세포 증식능 활성화, 골 대사와 연관있는 대표적 사이토카인인 IL-6와 TNF-${\alpha}$ 분비 억제 및 조절 등을 들 수 있다. 뿐만 아니라, 체중 증가량을 조절하는 역할을 하는 것으로 관찰되었다. 따라서 청국장 배합 사료는 난소적출 마우스 면역계의 조절 기전에 작용하여 면역세포 활성을 촉진시키고 효과적으로 작용할 수 있으리라 사료된다. 이러한 연구 결과를 토대로 기능성 식품 개발에 기초연구 자료가 될 것으로 기대되며 향후 청국장의 면역 활성물질의 분리 및 동정을 위한 연구의 뒷받침이 될 수 있을 것으로 생각된다.

• Asian-Australasian Journal of Animal Sciences
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• 제13권10호
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• pp.1414-1421
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• 2000

Sixteen specific pathogen free 4-wk-old crossbred weanling pigs were allotted into a $2{\times}2$ factorial experiment to evaluate the effects of chromium (Cr) on the immune responses after lipopolysaccharide (LPS) injection. Two factors included (1) no Cr or 400 ppb Cr supplementation from chromium picolinate (CrPic) and (2) LPS injection ($200{\mu}g/kg$ BW, intraperitoneally) on day 21 (d 21) and 35 (d 35) as compared with saline application. Plasma samples were obtained from all piglets before (0 h) and at 2 h, 4 h, 8 h, and 24 h after LPS injection. The changes in tumor necrosis $factor-{\alpha}$ ($TNF-{\alpha}$) and leukocyte populations after LPS injection were not significant on d 21. On d 35, the plasma $TNF-{\alpha}$ level was increased at h 2 postinjection, and supplemental Cr reduced the $TNF-{\alpha}$ level. The leukocyte populations had changed profoundly and lymphocyte subsets of $CD2^+$ and $CD8^+$ were reduced at 8 h postinjection. The blood granulocytes were increased and the percentage of $CD2^+$ was reduced in the Cr-fed group on d 35. Furthermore, Cr supplementation decreased the blastogensis of concanavalin A-stimulated peripheral blood mononuclear cells (PBMC) on d 21. These results suggest that 400 ppb Cr supplementation from CrPic in diets may modulate the immune responses in weanling pigs during LPS injection.

• Molecules and Cells
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• 제39권6호
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• pp.468-476
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• 2016

PLZF-expressing invariant natural killer T cells and CD4 T cells are unique subsets of innate T cells. Both are selected via thymocyte-thymocyte interaction, and they contribute to the generation of activated/memory-like CD4 and CD8 T cells in the thymus via the production of IL-4. Here, we investigated whether $PLZF^+$ innate T cells also affect the development and function of $Foxp3^+$ regulatory CD4 T cells. Flow cytometry analysis of the thymus and spleen from both CIITA transgenic C57BL/6 and wild-type BALB/c mice, which have abundant $PLZF^+$ CD4 T cells and invariant natural killer T cells, respectively, revealed that $Foxp3^+$ T cells in these mice exhibited a $CD103^+$ activated/memorylike phenotype. The frequency of $CD103^+$ regulatory T cells was considerably decreased in $PLZF^+$ cell-deficient $CIITA^{Tg}Plzf^{lu/lu}$ and $BALB/c.CD1d^{-/-}$ mice as well as in an IL-4-deficient background, such as in $CIITA^{Tg}IL-4^{-/-}$ and $BALB/c.IL-4^{-/-}$ mice, indicating that the acquisition of an activated/ memory-like phenotype was dependent on $PLZF^+$ innate T cells and IL-4. Using fetal thymic organ culture, we further demonstrated that IL-4 in concert with TGF-${\beta}$ enhanced the acquisition of the activated/memory-like phenotype of regulatory T cells. In functional aspects, the activated/ memory-like phenotype of Treg cells was directly related to their suppressive function; regulatory T cells of $CIITA^{Tg}PIV^{-/-}$ mice more efficiently suppressed ovalbumin-induced allergic airway inflammation compared with their counterparts from wild-type mice. All of these findings suggest that $PLZF^+$ innate T cells also augmented the generation of activated/memory-like regulation via IL-4 production.