首页> 美国卫生研究院文献>other >Altered Ratio of T Follicular Helper Cells to T Follicular Regulatory Cells Correlates with Autoreactive Antibody Response in Simian Immunodeficiency Virus–Infected Rhesus Macaques
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Altered Ratio of T Follicular Helper Cells to T Follicular Regulatory Cells Correlates with Autoreactive Antibody Response in Simian Immunodeficiency Virus–Infected Rhesus Macaques

机译:T滤泡辅助细胞与T滤泡调节细胞比例的改变与猿猴免疫缺陷病毒感染的猕猴的自身反应性抗体反应相关

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摘要

Individuals with chronic HIV-1 infection have an increased prevalence of autoreactive Abs. Many of the isolated HIV broadly neutralizing Abs from these individuals are also autoreactive. However, the underlying mechanism(s) that produce these autoreactive broadly neutralizing Abs remains largely unknown. The highly regulated coordination among B cells, T follicular helper (TFH) cells, and T follicular regulatory (TFR) cells in germinal centers (GCs) of peripheral lymphatic tissues (LTs) is essential for defense against pathogens while also restricting autoreactive responses. We hypothesized that an altered ratio of TFH/TFR cells in the GC contributes to the increased prevalence of autoreactive Abs in chronic HIV infection. We tested this hypothesis using a rhesus macaque (RM) SIV model. We measured the frequency of TFH cells, TFR cells, and GC B cells in LTs and anti-dsDNA and anti-phospholipid Abs from Indian RMs, with and without SIV infection. We found that the frequency of anti-dsDNA and anti-phospholipid Abs was much higher in chronically infected RMs (83.3% [5/6] and 66.7% [4/6]) than in acutely infected RMs (33.3% [2/6] and 18.6% [1/6]) and uninfected RMs (0% [0/6] and 18.6% [1/6]). The increased ratio of TFH/TFR cells in SIV infection correlated with anti-dsDNA and anti-phospholipid autoreactive Ab levels, whereas the frequency of TFR cells alone did not correlate with the levels of autoreactive Abs. Our results provide direct evidence that the ratio of TFH/TFR cells in LTs is critical for regulating autoreactive Ab production in chronic SIV infection and possibly, by extension, in chronic HIV-1 infection.
机译:患有慢性HIV-1感染的人自身反应性Abs患病率增加。从这些个体中分离出的许多广泛中和抗体的HIV也具有自身反应性。然而,产生这些自反应性广泛中和抗体的潜在机制仍然未知。外周淋巴组织(LTs)的生发中心(GC)中的B细胞,T滤泡辅助(TFH)细胞和T滤泡调节(TFR)细胞之间高度调节的协调对于防御病原体至关重要,同时也限制了自身反应性。我们假设,GC中TFH / TFR细胞比例的改变会导致慢性HIV感染中自身反应性Abs的患病率增加。我们使用恒河猴(RM)SIV模型测试了这一假设。我们测量了有和没有SIV感染的印度RM中LTs,抗dsDNA和抗磷脂抗体中TFH细胞,TFR细胞和GC B细胞的频率。我们发现,慢性感染的RMs(83.3%[5/6]和66.7%[4/6])的抗dsDNA和抗磷脂抗体的频率比急性感染的RMs(33.3%[2/6]高得多]和18.6%[1/6])和未感染的RM(0%[0/6]和18.6%[1/6])。 SIV感染中TFH / TFR细胞比例的增加与抗dsDNA和抗磷脂的自身反应性抗体水平相关,而单独的TFR细胞的频率与自身反应性抗体水平无关。我们的结果提供了直接的证据,即LTs中TFH / TFR细胞的比例对于调节慢性SIV感染以及可能进一步扩大的慢性HIV-1感染中自身反应性Ab产生至关重要。

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