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AASLD2018[575]575 免疫细胞效应器需要 不同流通和清算的清关 肝 [复制链接]

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发表于 2018-10-26 15:08 |只看该作者 |倒序浏览 |打印
575
Immune Cellular Effectors Required for the
Clearances of Different Circulating and
Intrahepatic HBV Antigens
Dan Zhu1, Jia Liu2 and Dongliang Yang2, (1)Department
of Infectious Disease, Union Hosipital,Tongji Medical
College,Huazhong University of Science and Technology,
(2)Department of Infectious Disease, Union Hospital, Tongji
Medical College, Huazhong University of Science and
Technology
Background: Both HBsAg and HBeAg serve as important
serologic markers for the diagnosis and monitoring of patients
with chronic hepatitis B. A cure for HBV infection is most
specifically indicated by HBsAg seroconversion, which usually
occurs later than HBeAg seroconversion. In clinical practice,
however, some patients with HBsAg seroconversion were
found to be persistently positive for circulating HBeAg and
HBV DNA, as well as intrahepatic HBV antigens and DNA.
These observations suggest that different immune effectors
are responsible for the clearances of different circulating and
intrahepatic HBV antigens Methods: To better define the
possible mechanisms, the clearances of HBsAg, HBeAg,
HBcAg and HBV DNA in the serum and liver were studied in
mice that were temporarily depleted a panel of immune cells and
challenged with HBV through hydrodynamic injection (HDI).
Results: We could demonstrate that in the HBV HDI mouse
model, serum HBV DNA clearance is associated with serum
HBeAg clearance but not HBsAg seroconversion. Intrahepatic
HBsAg remains positive after HBsAg seroconversion, while
the clearances of intrahepatic HBcAg and serum HBeAg are
synchronous. Depletion of CD8 T cells resulted in persistence
of serum HBeAg and HBV DNA, but only a slight delay of
HBsAg seroconversion. In contrast, depletion of CD4 T cells
or B cells resulted in persistence of serum HBsAg, HBeAg
and HBV DNA. Interestingly, clearance of intrahepatic HBsAg
but not HBcAg was observed in B cell depleted mice, although
they remained serum HBsAg positive at the corresponding
time point. To further examine the function of CD8 T cells and
B cells in mediating serum HBsAg and HBeAg, purified CD8
T cells and non-CD8 splenocytes (about 60% of which are B
cells) from HBV resolved mice were adoptively transferred to
naive mice. CD8 T cells preferentially infiltrated into the liver
while B cells preferentially infiltrated into the spleen. After HBV
challenge, CD8 T cell transferred mice showed significantly
accelerated serum HBeAg clearance and non-CD8
splenocyte transferred mice showed significantly accelerated
serum HBsAg clearance. Conclusion: Taken together, these
results reveal that CD8+ T cells are not essential cellular
effector for circulating HBsAg clearance. Both CD4 T cells
and B cells serve as master effectors for circulating HBsAg,
HBeAg and HBV DNA clearances. The role and mechanism
of B cells in mediating intrahepatic HBV clearance remains to
be thoroughly explored.

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发表于 2018-10-26 15:09 |只看该作者
575
免疫细胞效应器需要
不同流通和清算的清关
肝内HBV抗原
Dan Zhu,Jia Liu2和Dongliang Yang2,(1)部
传染病,Union Hosipital,同济医疗
华中科技大学学院
(2)同济市协和医院传染病科
华中科技大学医学院
技术
背景:HBsAg和HBeAg都很重要
用于诊断和监测患者的血清学标志物
慢性乙型肝炎。最常见的是治疗HBV感染
通常由HBsAg血清转换特异性表明
发生晚于HBeAg血清学转换。在临床实践中,
然而,一些HBsAg血清学转换患者是
发现HBeAg循环持续阳性
HBV DNA,以及肝内HBV抗原和DNA。
这些观察结果表明不同的免疫效应物
负责不同流通和清关的清关
肝内HBV抗原方法:更好地定义
可能的机制,HBsAg,HBeAg的清除,
研究血清和肝脏中的HBcAg和HBV DNA
暂时耗尽一组免疫细胞的小鼠
通过流体动力学注射(HDI)对HBV提出挑战。
结果:我们可以证明在HBV HDI小鼠中
模型,血清HBV DNA清除率与血清有关
HBeAg清除但不是HBsAg血清转换。肝内
HBsAg血清转换后HBsAg仍为阳性,而
肝内HBcAg和血清HBeAg的清除率为
同步。 CD8 T细胞的消耗导致持久性
血清HBeAg和HBV DNA,但只有轻微的延迟
HBsAg血清学转换。相反,CD4 T细胞耗尽
或B细胞导致血清HBsAg,HBeAg持续存在
和HBV DNA。有趣的是,清除肝内HBsAg
但是,在B细胞耗尽的小鼠中没有观察到HBcAg
他们在相应的血清HBsAg阳性
时间点。进一步检查CD8 T细胞的功能
B细胞介导血清HBsAg和HBeAg,纯化CD8
T细胞和非CD8脾细胞(其中约60%是B
将来自HBV解析小鼠的细胞过继转移至
天真的老鼠。 CD8 T细胞优先渗入肝脏
而B细胞优先渗入脾脏。 HBV之后
挑战,CD8 T细胞转移小鼠显示明显
加速血清HBeAg清除和非CD8
脾细胞转移小鼠显示明显加速
血清HBsAg清除率。结论:综合起来,这些
结果显示CD8 + T细胞不是必需的细胞
用于循环HBsAg清除的效应器。两种CD4 T细胞
和B细胞作为循环HBsAg的主效应物,
HBeAg和HBV DNA清除率。角色和机制
B细胞在介导肝内HBV清除中的作用仍然存在
彻底探索。
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