The Role of Defensins in HIV Pathogenesis

Profound loss of CD4+T cells, progressive impairment of the immune system, inflammation, and sustained immune activation are the characteristics of human immunodeficiency virus-1 (HIV-1) infection. Innate immune responses respond immediately from the day of HIV infection, and a thorough understanding of the interaction between several innate immune cells and HIV-1 is essential to determine to what extent those cells play a crucial role in controlling HIV-1in vivo. Defensins, divided into the three subfamiliesα-,β-, andθ-defensins based on structure and disulfide linkages, comprise a critical component of the innate immune response and exhibit anti-HIV-1 activities and immunomodulatory capabilities. In humans, onlyα- andβ-defensins are expressed in various tissues and have broad impacts on HIV-1 transmission, replication, and disease progression.θ-defensins have been identified as functional peptides in Old World monkeys, but not in humans. Instead,θ-defensins exist only as pseudogenes in humans, chimpanzees, and gorillas. The use of the syntheticθ-defensin peptide “retrocyclin” as an antiviral therapy was shown to be promising, and further research into the development of defensin-based HIV-1 therapeutics is needed. This review focuses on the role of defensins in HIV-1 pathogenesis and highlights future research efforts that warrant investigation.

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From Capsids to Complexes: Expanding the Role of TRIM5α in the Restriction of Divergent RNA Viruses and Elements

Viruses ◽

10.3390/v13030446 ◽

2021 ◽

Vol 13 (3) ◽

pp. 446

Author(s):

Kevin M. Rose ◽

Stephanie J. Spada ◽

Rebecca Broeckel ◽

Kristin L. McNally ◽

Vanessa M. Hirsch ◽

...

Keyword(s):

Human Immunodeficiency Virus ◽

Molecular Basis ◽

Human Population ◽

Rna Viruses ◽

Arms Race ◽

Innate Immune ◽

Immunodeficiency Virus ◽

Underlying Mechanisms ◽

Hiv 1

An evolutionary arms race has been ongoing between retroviruses and their primate hosts for millions of years. Within the last century, a zoonotic transmission introduced the Human Immunodeficiency Virus (HIV-1), a retrovirus, to the human population that has claimed the lives of millions of individuals and is still infecting over a million people every year. To counteract retroviruses such as this, primates including humans have evolved an innate immune sensor for the retroviral capsid lattice known as TRIM5α. Although the molecular basis for its ability to restrict retroviruses is debated, it is currently accepted that TRIM5α forms higher-order assemblies around the incoming retroviral capsid that are not only disruptive for the virus lifecycle, but also trigger the activation of an antiviral state. More recently, it was discovered that TRIM5α restriction is broader than previously thought because it restricts not only the human retroelement LINE-1, but also the tick-borne flaviviruses, an emergent group of RNA viruses that have vastly different strategies for replication compared to retroviruses. This review focuses on the underlying mechanisms of TRIM5α-mediated restriction of retroelements and flaviviruses and how they differ from the more widely known ability of TRIM5α to restrict retroviruses.

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Human Immunodeficiency Virus Inhibits Multilineage Hematopoiesis In Vivo

Journal of Virology ◽

10.1128/jvi.72.6.5121-5127.1998 ◽

1998 ◽

Vol 72 (6) ◽

pp. 5121-5127 ◽

Cited By ~ 42

Author(s):

Prasad S. Koka ◽

John K. Fraser ◽

Yvonne Bryson ◽

Gregory C. Bristol ◽

Grace M. Aldrovandi ◽

...

Keyword(s):

Human Immunodeficiency Virus ◽

Progenitor Cells ◽

Ex Vivo ◽

Erythroid Differentiation ◽

Inhibitory Effect ◽

Immunodeficiency Virus ◽

The Many ◽

Hiv 1

ABSTRACT Human immunodeficiency virus type 1 (HIV-1)-infected individuals often exhibit multiple hematopoietic abnormalities reaching far beyond loss of CD4+ lymphocytes. We used the SCID-hu (Thy/Liv) mouse (severe combined immunodeficient mouse transplanted with human fetal thymus and liver tissues), which provides an in vivo system whereby human pluripotent hematopoietic progenitor cells can be maintained and undergo T-lymphoid differentiation and wherein HIV-1 infection causes severe depletion of CD4-bearing human thymocytes. Herein we show that HIV-1 infection rapidly and severely decreases the ex vivo recovery of human progenitor cells capable of differentiation into both erythroid and myeloid lineages. However, the total CD34+ cell population is not depleted. Combination antiretroviral therapy administered well after loss of multilineage progenitor activity reverses this inhibitory effect, establishing a causal role of viral replication. Taken together, our results suggest that pluripotent stem cells are not killed by HIV-1; rather, a later stage important in both myeloid and erythroid differentiation is affected. In addition, a primary virus isolated from a patient exhibiting multiple hematopoietic abnormalities preferentially depleted myeloid and erythroid colony-forming activity rather than CD4-bearing thymocytes in this system. Thus, HIV-1 infection perturbs multiple hematopoietic lineages in vivo, which may explain the many hematopoietic defects found in infected patients.

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Structure-Based Design and Engineering of a Nontoxic Recombinant Pokeweed Antiviral Protein with Potent Anti-Human Immunodeficiency Virus Activity

Antimicrobial Agents and Chemotherapy ◽

10.1128/aac.47.3.1052-1061.2003 ◽

2003 ◽

Vol 47 (3) ◽

pp. 1052-1061 ◽

Cited By ~ 13

Author(s):

Fatih M. Uckun ◽

Francis Rajamohan ◽

Sharon Pendergrass ◽

Zahide Ozer ◽

Barbara Waurzyniak ◽

...

Keyword(s):

Human Immunodeficiency Virus ◽

Scid Mouse ◽

Pokeweed Antiviral Protein ◽

Antiviral Protein ◽

Immunodeficiency Virus ◽

Scid Mouse Model ◽

Anti Hiv ◽

Hiv 1

ABSTRACT A molecular model of pokeweed antiviral protein (PAP)-RNA interactions was used to rationally engineer FLP-102(151AA152) and FLP-105(191AA192) as nontoxic PAPs with potent anti-human immunodeficiency virus (anti-HIV) activities. FLP-102 and FLP-105 have been produced in Escherichia coli and tested both in vitro and in vivo. These proteins depurinate HIV type 1 (HIV-1) RNA much better than rRNA and are more potent anti-HIV agents than native PAP or recombinant wild-type PAP. They are substantially less toxic than native PAP in BALB/c mice and exhibit potent in vivo activities against genotypically and phenotypically nucleoside reverse transcriptase inhibitor-resistant HIV-1 in a surrogate human peripheral blood lymphocyte (Hu-PBL) SCID mouse model of human AIDS. Rationally engineered nontoxic recombinant PAPs such as FLP-102 and FLP-105 may provide the basis for effective salvage therapies for patients harboring highly drug-resistant strains of HIV-1. The documented in vitro potencies of FLP-102 and FLP-105, their in vivo antiretroviral activities in the HIV-infected Hu-PBL SCID mouse model, and their favorable toxicity profiles in BALB/c mice warrant the further development of these promising new biotherapeutic agents.

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Structure-Activity Relationship Studies on Potential Non-Nucleoside DABO-Like Inhibitors of HIV-1 Reverse Transcriptase

Antiviral Chemistry and Chemotherapy ◽

10.1177/095632020001100204 ◽

2000 ◽

Vol 11 (2) ◽

pp. 117-133 ◽

Cited By ~ 10

Author(s):

Roberta Costi ◽

Roberto Di Santo ◽

Marino Artico ◽

Silvio Massa ◽

Antonio Lavecchia ◽

...

Keyword(s):

Reverse Transcriptase ◽

Structure Activity Relationship ◽

Activity Relationship ◽

Enzyme Assays ◽

Structure Activity ◽

Immunodeficiency Virus ◽

Anti Hiv ◽

Hiv 1

Using 2,6-dichloro-4-aminopyrimidine, a number of uracil and cytosine derivatives with both arylthio and alkoxy moieties were prepared. These novel pyrimidines share chemical similarities with DABOs and HEPTs, two classes of nonnucleoside human immunodeficiency virus type 1 (HIV-1) reverse transcriptase inhibitors (NNRTIs), which have been widely studied of late. All new derivatives were tested in MT-4 cells to explore their potential in vivo anti-HIV activity. Like other NNRTIs, they selectively inhibit HIV-1 but not HIV- 2. The majority of test derivatives were found to have low potency and were sometimes more cytotoxic than zidovudine and emivirine (formerly MKC-442), used here as reference drugs. Uracil and cytosine derivatives bearing a sec-butoxy chain and a methyl-substituted benzenesulphonyl moiety were the most potent. Enzyme assays proved that these derivatives target RT. Structure-activity relationship studies established a correlation between the anti-HIV-1 activity and the meta substitution on the phenyl ring; furthermore, oxidation of sulphide to sulphone significantly increased the potency of certain derivatives.

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In Vivo Toxicity, Pharmacokinetics, and Anti-Human Immunodeficiency Virus Activity of Stavudine-5′-(p-Bromophenyl Methoxyalaninyl Phosphate) (Stampidine) in Mice

Antimicrobial Agents and Chemotherapy ◽

10.1128/aac.46.11.3428-3436.2002 ◽

2002 ◽

Vol 46 (11) ◽

pp. 3428-3436 ◽

Cited By ~ 27

Author(s):

Fatih M. Uckun ◽

Sanjive Qazi ◽

Sharon Pendergrass ◽

Elizabeth Lisowski ◽

Barbara Waurzyniak ◽

...

Keyword(s):

Human Immunodeficiency Virus ◽

Human Peripheral Blood ◽

Pharmacokinetic Profile ◽

Transcriptase Inhibitor ◽

Immunodeficiency Virus ◽

Dose Levels ◽

Anti Hiv ◽

Hiv 1

ABSTRACT We have evaluated the clinical potential of stavudine-5′-(p-bromophenyl methoxyalaninyl phosphate(stampidine [STAMP]), a novel aryl phosphate derivative of stavudine, as a new anti-human immunodeficiency virus (anti-HIV) agent, by examining its acute, subacute, and chronic toxicity profile in mice as well as by testing its antiviral activity in a surrogate human peripheral blood lymphocyte (Hu-PBL)-SCID mouse model of human AIDS. STAMP was very well tolerated in BALB/c and CD-1 mice, without any detectable acute or subacute toxicity at single intraperitoneal or oral bolus doses as high as 500 mg/kg of body weight. Notably, daily administration of STAMP intraperitoneally or orally for up to 8 consecutive weeks was not associated with any detectable toxicity at cumulative dose levels as high as 6.4 g/kg. Micromolar concentrations of the active STAMP metabolite in plasma were rapidly achieved and maintained for more than 4 h after parenteral as well as oral administration of a nontoxic 100-mg/kg bolus dose of STAMP. In accordance with its favorable pharmacokinetic profile and in vitro potency, STAMP exhibited dose-dependent and potent in vivo anti-HIV activity in Hu-PBL-SCID mice against a genotypically and phenotypically nucleoside analog reverse transcriptase inhibitor (NRTI)-resistant clinical HIV type 1 (HIV-1) isolate (BR/92/019; D67N, L214F, T215D, K219Q) at nontoxic dose levels. The remarkable in vivo safety and potency of STAMP warrants the further development of this promising new antiretroviral agent for possible clinical use in patients harboring NRTI-resistant HIV-1.

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HARNESSING INNATE IMMUNE RESPONSES TO ENHANCE ANTI-HIV-1 THERAPIES

Medical Research Archives ◽

10.18103/mra.v0i3.285 ◽

2015 ◽

Author(s):

Alexandra L Howell

Keyword(s):

Immune Responses ◽

Innate Immune ◽

Innate Immune Responses ◽

Anti Hiv ◽

Hiv 1

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Lentiviral Vectors Interfering with Virus-Induced CD4 Down-Modulation Potently Block Human Immunodeficiency Virus Type 1 Replication in Primary Lymphocytes

Journal of Virology ◽

10.1128/jvi.78.23.13072-13081.2004 ◽

2004 ◽

Vol 78 (23) ◽

pp. 13072-13081 ◽

Cited By ~ 26

Author(s):

Hang M. Pham ◽

Enrique R. Argañaraz ◽

Bettina Groschel ◽

Didier Trono ◽

Juan Lama

Keyword(s):

Human Immunodeficiency Virus ◽

Lentiviral Vectors ◽

Viral Pathogenesis ◽

Viral Particles ◽

Immunodeficiency Virus ◽

Anti Hiv ◽

Hiv 1

ABSTRACT CD4 down-modulation is essential for the production of human immunodeficiency virus (HIV) infectious particles. Disease progression correlates with enhanced viral induced CD4 down-modulation, and a subset of long-term nonprogressors carry viruses defective in this function. Despite multiple pieces of evidence highlighting the importance of this function in viral pathogenesis in vivo, to date, HIV-induced CD4 down-modulation has not been used as a target for intervention. We describe here HIV-based vectors that deliver truncated CD4 molecules resistant to down-modulation by the viral products Nef and Vpu. Infection of cells previously transduced with these vectors proceeded normally, and viral particles were released in normal amounts. However, the infectivity of the released virions was reduced 1,000-fold. Lentiviral vectors expressing truncated CD4 molecules were efficient at blocking HIV-1 infectivity and replication in several cell lines and in CD4-positive primary lymphocytes. The findings presented here provide proof-of-principle that approaches targeting the virus-induced CD4 down-modulation may constitute the basis for novel anti-HIV therapies.

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Polyethylene Glycol 40-Modified Peptide with High Therapeutic Efficacy in Simian-Human Immunodeficiency Virus-Acutely Infected Rhesus Monkeys

Journal of Virology ◽

10.1128/jvi.00386-20 ◽

2020 ◽

Vol 94 (14) ◽

Cited By ~ 1

Author(s):

Mingli Li ◽

Shuihong Cheng ◽

Yibo Ding ◽

Chen Wang ◽

Yong Feng ◽

...

Keyword(s):

Human Immunodeficiency Virus ◽

Half Life ◽

Rhesus Monkeys ◽

Glycosylation Site ◽

Control Treatment ◽

Immunodeficiency Virus ◽

Anti Hiv ◽

Hiv 1

ABSTRACT Anti-human immunodeficiency virus type 1 (anti-HIV-1) fusion peptides have been studied for nearly 2 decades, but few candidates have found useful clinical applications. One factor underlying the failure of such agents to reach the clinic is their poor pharmacokinetic properties, and many efforts have been made to overcome this problem. In this study, we modified C34, a peptide inhibitor of HIV-1 fusion, at its conserved glycosylation site using polyethylene glycols (PEGs) of different molecular weights. PEG40-NC, a conjugate of C34 and branched PEG 40 kDa (PEG40), which has been previously shown to improve the pharmacokinetic profiles of proteins, showed a significantly extended half-life (t1/2; 10.39 h in rats), which compensated for decreased in vitro activity (50% effective concentration [EC50] of 18.51 nM). PEG40-NC also showed a mechanism of action similar to that of C34. PEG40-NC monotherapy in acutely simian-human immunodeficiency virus (SHIV)-infected rhesus monkeys significantly suppressed viral load compared with a control treatment. Efficacy was linked to the extended half-life and lymphatic exposure conferred by attached PEG40. These results highlight the potential of further clinical investigations of PEG40-NC in combination with antiretroviral therapy or other anti-HIV agents. IMPORTANCE Poor pharmacokinetics have severely hindered the clinical use of anti-HIV peptides. Different small molecules, such as lipid, cholesterol, and small PEG, were designed to modify peptides to improve their pharmacokinetics. In this study, we incorporated large branched PEG to anti-HIV peptide and obtained a conjugate with extended half-life and improved in vivo efficacy. The strategy we developed in this study can also be applicable for the development of other peptide candidates.

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In Vivo Role of TLR2 and MyD88 Signaling in Eliciting Innate Immune Responses in Staphylococcal Endophthalmitis

Investigative Ophthalmology & Visual Science ◽

10.1167/iovs.14-16087 ◽

2015 ◽

Vol 56 (3) ◽

pp. 1719-1732 ◽

Cited By ~ 30

Author(s):

D. Talreja ◽

P. K. Singh ◽

A. Kumar

Keyword(s):

Immune Responses ◽

Innate Immune ◽

Innate Immune Responses ◽

Myd88 Signaling

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Mitochondrial antiviral signalling protein is crucial for the development of pulmonary fibrosis

European Respiratory Journal ◽

10.1183/13993003.00652-2020 ◽

2020 ◽

pp. 2000652

Author(s):

Sang-Hun Kim ◽

Jung Yeon Lee ◽

Chang Min Yoon ◽

Hyeon Jun Shin ◽

Sei Won Lee ◽

...

Keyword(s):

Pulmonary Fibrosis ◽

Therapeutic Strategy ◽

Innate Immune ◽

Therapeutic Effects ◽

Innate Immune Responses ◽

Approved Drugs ◽

Molecular Patterns ◽

Damage Associated Molecular Patterns

Danger signals, or damage-associated molecular patterns (DAMPs), instigate mitochondrial innate immune responses wherein Mitochondrial Antiviral Signalling protein (MAVS) functions as a key platform molecule to mediate them. The role of MAVS in the pathogenesis of idiopathic pulmonary fibrosis (IPF), however, has not been identified yet. A possibility whether the MAVS signalling can be modulated by currently existing drugs has not been explored, either. Here, using an established model of pulmonary fibrosis, we demonstrate that MAVS plays as a critical mediator of multiple DAMPs signalling pathways and the consequent lung fibrosis after bleomycin-induced injury in vivo. After bleomycin injury, the expression of MAVS was mainly observed in macrophages. In addition, multimeric MAVS aggregation, a key event of MAVS signalling activation, was significantly increased and persisted in bleomycin-injured lungs. Interestingly, a proapoptotic BH3 mimetic ABT-263 attenuated the expression of MAVS and its signalling and, consequently, the development of experimental pulmonary fibrosis. In contrast, the therapeutic effects of Pirfenidone or Nintedanib, two approved drugs for IPF treatment, were not related to the modulation of MAVS or its signalling. Importantly, multimeric MAVS aggregation was significantly increased in lungs from the patients with IPF as well. In conclusion, MAVS may play an important role in the development of pulmonary fibrosis, and targeting MAVS with BH3 mimetics may provide a novel therapeutic strategy for IPF, a major unmet disorder.

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