Complement and HIV-I infection/HIV-associated neurocognitive disorders

Liu, Fengming; Dai, Sheng; Gordon, Jennifer; Qin, Xuebin

doi:10.1007/s13365-014-0243-9

Cited by 23 publications

(34 citation statements)

References 131 publications

(161 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…It is confirmed that HIV-1 virions isolated from infected individuals have accumulated C3 on their surface, a signal of the initiation of complement reactions, but HIV-1 virions are still very resistant to complement mediated killing, which is a different phenomenon of humoral immune responses induced from the most invaded pathogens [32]. More and more experimental and clinical evidences indicate that MAC pores supposed to be seen on the surface of invaded pathogen are not effectively formed in the case of HIV infection, leading to the escape of virus and all over spreading through the blood and lymph systems in HIV patients [53,54].…”

Section: Critical Role Of Fh In Pathogenesis Of Several Dreadful Disementioning

confidence: 99%

“…The complement-mediated lysis could be further enhanced through the addition of a blocking antibody against CD55; however, FH binding was shown to be responsible for most of the resistance mechanism in both cases. It has been confirmed that resistance to human complement can be completely overcome if Decay accelerating factor (DAF)/CD55 and FH are set out of function [32, 53,54].…”

Section: Critical Role Of Fh In Pathogenesis Of Several Dreadful Disementioning

confidence: 99%

See 1 more Smart Citation

Age to End Dreadful Diseases (HIV, Malaria, TB, Cancer and More): A Theory of Intact or Protected Complement (IPC) Immunity

Jin¹

2017

J Vaccines Vaccin

View full text Add to dashboard Cite

After enormous efforts to fight for a successful HIV vaccine, the movement ended with frustration. While people are celebrating the victories of disease prophylaxis and healthy improvement, millions of them are still struggling on numerous unsettled dreadful illnesses, i.e., HIV, malaria, TB, cancer and autoimmune disorders. A theory of Intact or Protected Complement (IPC) immunity proposed in this review is to focus on hijacked complement system, the powerful leverage weapon restrained by many pathogens or cancer cells. The theory is to stimulate more investigations to discover the key block in continuous achievement in successful vaccine development and immune therapy.

show abstract

Section: Critical Role Of Fh In Pathogenesis Of Several Dreadful Disementioning

confidence: 99%

Section: Critical Role Of Fh In Pathogenesis Of Several Dreadful Disementioning

confidence: 99%

Age to End Dreadful Diseases (HIV, Malaria, TB, Cancer and More): A Theory of Intact or Protected Complement (IPC) Immunity

Jin¹

2017

J Vaccines Vaccin

View full text Add to dashboard Cite

show abstract

“…Natural killer cell activation is present in the setting of HIV and does not normalize despite virologic suppression during cART (Lichtfuss et al, 2012). Additionally, activation of the complement system has been recognized since the early years of the HIV epidemic (Liu et al, 2014, Senaldi et al, 1990). It is possible that the complement system plays a role in HIV neuropathogenesis.…”

Section: Introductionmentioning

confidence: 99%

Soluble membrane attack complex in the blood and cerebrospinal fluid of HIV-infected individuals, relationship to HIV RNA, and comparison with HIV negatives

Anderson

Schein

Kalapila

et al. 2017

Journal of Neuroimmunology

View full text Add to dashboard Cite

The soluble membrane attack complex (sMAC) represents the terminal product of the complement cascade. We enrolled 47 HIV+ adults (12 of whom underwent a second visit at least 24 weeks after starting therapy) as well as 11 HIV negative controls. At baseline, cerebrospinal fluid (CSF) sMAC was detectable in 27.7% of HIV+ individuals. CSF sMAC correlated with CSF HIV RNA levels and was more likely to be detectable in HIV+ individuals on cART compared to HIV negative controls. In HIV+ participants, there were negative association trends between sMAC and neurocognitive performance but these did not reach statistical significance.

show abstract

“…Complement is activated early in HIV infection via a variety of mechanisms, but it fails to eradicate HIV from infected cells and from the circulation due to the presence of complement regulators within the HIV-1 envelope and on infected cells (Liu et al 2014). Instead, HIV uses complement activation to spread and enhance systemic infection (Liu et al 2014). The role of complement in the neuropathogenesis of HIV is less well understood.…”

Section: Introductionmentioning

confidence: 99%

“…The role of complement in the neuropathogenesis of HIV is less well understood. Local HIV infection induces C3 production in neuronal and glial cell lines incubated with HIV and in parallel downregulates normal complement inhibitor proteins (CD59) (Stephan et al 2012; Liu et al 2014). In a simian immunodeficiency virus (SIV) model, cerebral synthesis of C1q and C3 was upregulated compared to controls and deposited on neuronal membranes (Speth et al 2004).…”

Section: Introductionmentioning

confidence: 99%

The complement system, neuronal injury, and cognitive function in horizontally-acquired HIV-infected youth

et al. 2016

View full text Add to dashboard Cite

The complement system (C1q/C3) is a key mediator of synaptic pruning during normal development. HIV inappropriately induces C1q and C3 production in the brain, and reduces neuronal complement inhibition. HIV may thus alter neural connectivity in the developing brain by excessively targeting synapses for elimination. The resultant pattern of neuronal injury may fundamentally alter neurodevelopmental and cognitive processes differentially across ages. This study aimed to (1) measure the association between the cerebrospinal fluid (CSF) complement factors (C1q/C3) and a marker of neuronal injury (NFL) in HIV+ subjects; (2) quantify the differences in CSF C1q/C3 between HIV+ youth and older adults; and (3) define the relationship between CSF C1q/C3 and cognitive impairment in each age group. We performed a retrospective cross-sectional study of 20 HIV+ 18–24-year-old youth and 20 HIV+ 40–46-year-old adults with varying levels of cognitive impairment enrolled in the CNS Antiretroviral Therapy Effects Research study. We quantified C3, C1q, and NFL by ELISA in paired CSF/plasma specimens. We found that CSF C1q correlates with NFL in all subjects not receiving antiretroviral therapy (n = 16, rho = 0.53, p = 0.035) when extreme NFL outliers were eliminated (n = 1). There was no difference in plasma/CSF C1q or C3 between older adults and youth. In 18–24-year-old youth, a nearly significant (p = 0.052) elevation of CSF C1q expression was observed in cognitively impaired subjects compared to cognitively normal subjects. Further investigation into the role of the CNS complement system in the neuropathogenesis of HIV is warranted and should be considered in a developmentally specific context.

show abstract

Complement and HIV-I infection/HIV-associated neurocognitive disorders

Cited by 23 publications

References 131 publications

Age to End Dreadful Diseases (HIV, Malaria, TB, Cancer and More): A Theory of Intact or Protected Complement (IPC) Immunity

Age to End Dreadful Diseases (HIV, Malaria, TB, Cancer and More): A Theory of Intact or Protected Complement (IPC) Immunity

Soluble membrane attack complex in the blood and cerebrospinal fluid of HIV-infected individuals, relationship to HIV RNA, and comparison with HIV negatives

The complement system, neuronal injury, and cognitive function in horizontally-acquired HIV-infected youth

Contact Info

Product

Resources

About