Your search keyword '"gp41"' showing total 93 results

1. DNA adjuvant Amiloride conjunct long immunization interval promote higher antibody responses to HIV-1 gp41 and gp140 immunogens.

Author

Yao, Lan, Wang, Jia-Ye, Bao, Li-Na, Fan, Meng-Xuan, Bai, Yang, Chen, Wen-Jiang, Yuan, Chen, Yuan, Li, Wang, Jing, Li, Yan, Zhuang, Min, and Ling, Hong

Subjects

*ANTIBODY formation, *AMILORIDE, *HIV-1 glycoprotein 120, *HUMORAL immunity, *IMMUNIZATION

Abstract

• Amiloride as a DNA adjuvant can promote humoral immune responses after protein boosts. • Long immunization interval is benefit for the production of specific binding Abs. • Amiloride & long interval show better immune effect than elevating immunization times. • Q577A mutants of gp140 and gp41 show different immune effects compared to wild type. Recent studies have revealed that the interface of gp120 and gp41 and some parts of gp41 are also critical epitopes for elicitation of broadly neutralizing antibodies. Therefore, potential trimeric gp41 or gp140 immunogen candidates are needed. Previously, we developed a trimer motif MTQ and demonstrated that it could help formation of trimeric gp120 and gp140 proteins. In the present study, we immunized Balb/c mice using trimeric gp41-expressing plasmid for prime and monomeric gp41 or trimeric gp140 protein as well as a mutant (Q577A) for boost. The antibody responses in the context of regimens with various immunization intervals and DNA adjuvants including praziquantel (PZQ), cimetidine (CIM), and amiloride (AML) were evaluated. We found that these three adjuvants were not enough to elicit remarkable specific Abs after gp41 DNA immunization, while AML could significantly promote humoral immune responses after protein boosts. Long immunization interval could induce the specific binding Abs earlier and higher and maintain a high level of Abs in the following 27 weeks after final protein boost. Moreover, two times of protein boosts with DNA adjuvant and a longer time interval achieved a higher titer of specific Abs than three times of protein boosts with a shorter time interval. Q577A mutant was benefit for trimeric gp140 boost in the production of binding Abs but harmful to inducing neutralizing Abs, while this mutant in monomeric gp41 presented the opposite trend which may be associated with the immunogen structures. This study highlights the significance of DNA adjuvant Amiloride and long immunization interval in promoting antibody responses and provides new insights into effective HIV immunization regimen design in the future. [ABSTRACT FROM AUTHOR]

Published

2020

2. Characterization of HIV-1 genotype specific antigens for the detection of recent and long-term HIV-1 infection in China.

Author

Cai, Qundi, Wang, Haiying, Huang, Liping, Yan, Huanchang, Zhu, Wenchang, and Tang, Shixing

Subjects

*HIV, *GENOTYPES, *IMMUNOASSAY, *IMMUNOSPECIFICITY, *RECOMBINANT proteins

Abstract

Highlights • The sequences at the loop region of HIV-1 gp41 are essential for HIV incidence assay. • The impact of HIV-1 gene diversity on the incidence assay performance was confirmed. • HIV-1 incidence assay must use gp41 peptides specific for the predominant strains. Abstract To characterize HIV-1 gp41 as an antigen for developing HIV-1 incidence assay and to investigate the impact of HIV-1 genetic diversity on the assay performance, a number of truncated peptides were synthesized to identify the immunodominant epitopes (IDEs) of HIV-1 gp41 protein. Subsequently, the mixed peptides (MP3) or the recombinant protein (MP4) containing HIV-1 gp41 IDEs of the major HIV-1 genotype CRF01_AE, CRF07_BC/ CRF08_BC and subtype B in China were used to verify the sensitivity and specificity of HIV-1 recency testing. We identified the QKFLG and GKIIC motifs located in the loop region of HIV-1 gp41 as the two major IDEs. The surrounding amino acids EAQQHLLQLT and WNSSWSN could block the binding of gp41 peptide and anti-HIV antibody with low avidity, making the gp41 peptide p57 suitable for distinguishing recent and long-term HIV-1 infections. Furthermore, MP3 or MP4-based immunoassay could significantly improve the assay sensitivity and showed 93.33% (140/150) vs. 94.59% (35/37) and 94.08% (143/152) vs. 94.59% (35/37) concordance with commercially available LAg-Avidity EIA test among the cross-sectional and longitudinal samples, respectively. The estimated mean duration of recent infection (MDRI) was 130 days (95% CI: 83–167) and 166 days (95% CI: 123–202) for MP3 and MP4 assays, respectively. Our preliminary results indicate that the HIV-1 gp41 peptide-based immunoassay specifically targeting the major HIV-1 genotype CRF01_AE, CRF07_BC/CRF08_BC and subtype B could serve as a simple incidence assay for differentiating recent and long-term HIV-1 infections in China. [ABSTRACT FROM AUTHOR]

Published

2019

3. Gp41 inhibitory activity prediction of theaflavin derivatives using ligand/structure-based virtual screening approaches.

Author

Mostashari-Rad, Tahereh, Saghaei, Lotfollah, and Fassihi, Afshin

Subjects

*MOLECULAR docking, *DYNAMIC simulation

Abstract

Graphical abstract Highlights • Theaflavin digallate, a potent HIV-1 inhibitor, was considered as a template for ligand- and structure-based virtual screening approaches. • In silico Lipinski's Rule of Five and ADMET calculations, were performed to select the compounds with the best potential drug-like properties. • Molecular docking and molecular dynamic simulations were performed to select compounds with the best pharmacodynamic properties. • Some hits with possibly good anti-HIV activities and better pharmacokinetic properties than TF 3 were identified. • The selected compounds have balanced hydophilicity and lipophilicity and probably better gastrointestinal and blood brain barrier absorption. Abstract Gp41 and its conserved hydrophobic groove on the NHR region is one of the attractive targets in the design of HIV-1 entry inhibitory agents. This hydrophobic pocket is very critical for the progression of HIV and host cell fusion. In this study different ligand-based (structure similarity search) and structure-based (molecular docking and molecular dynamic simulation) methods were performed in a virtual screening procedure to select the best compounds with the most probable HIV-1 gp41 inhibitory activities. In silico pharmacokinetics and ADMET (absorption, distribution, metabolism, excretion and toxicity) properties filtration also was considered to choose the compounds with best drug-like properties. The results of molecular docking and molecular dynamic simulations of the final selected compounds showed suitable stabilities of their complexes with gp41. The final selected hits could have better pharmacokinetics properties than the template compound, theaflavin digallate (TF 3), a naturally-originated potent gp41 inhibitor. [ABSTRACT FROM AUTHOR]

Published

2019

4. Investigation of the inhibition effect of arachidonic acid on the core structure of the HIV-1 gp41.

Author

Xu, Xiaoying, Li, Lin, Liu, Zhen, Yao, Xiaojun, Zhang, Xuanxuan, Liu, Shuwen, and Liu, Lihong

Subjects

*ARACHIDONIC acid, *HIV infections, *GLYCOPROTEINS, *POLYACRYLAMIDE, *GEL electrophoresis

Abstract

Graphical abstract Highlights • Our study provides a new insight into the functional role of arachidonic acid during the formation of HIV-1 gp41 six-helix bundle. • Molecular docking techniques and isotherm titration microcalorimetry are adopted to explore the mechanism of kinetics. • AA presents the inhibitory activity to HIV-1JR-FL. Abstract The gp41 transmembrane domain of the envelope glycoprotein of the human immunodeficiency virus (HIV) modulates the conformation of the viral envelope spike. During the HIV fusion process, C-terminal heptad repeat (CHR, C34) wrap antiparallel to the N-terminal heptad repeat (NHR, N36) helices to form a stable six-helix bundle (6-HB) core structure, which brings the viral and cell membranes into close proximity for fusion. Therefore, inhibiting the formation of 6-HB is considered to be a key activity of an effective HIV-1 fusion inhibitor. The level of arachidonic acid (AA) is increased in HIV infected patients. Our study provides a new insight into the functional role of AA during the formation of HIV-1 gp41 6-HB. Native polyacrylamide gel electrophoresis (N-PAGE), enzyme-linked-immunosorbent serologic assay (ELISA) and circular dichroism (CD) spectroscopy were used to investigate the inhibition of AA for the formation of 6-HB. Molecular docking technique was adopted to explore the underlying mechanism. HIV-1 JR-FL (R5 strain) Envelope was adopted to determine the inhibition effect of AA. AA is shown to interfere with the formation of α-helical complexes of N36 and C34 by N-PAGE, ELISA and CD spectroscopy. The isotherm titration microcalorimetry (ITC) results indicate there is a single class of binding site on N36. ΔH and ΔS are −12.43 kJ mol−1 and 70.07 J mol−1 K−1, respectively, indicating hydrophobic interaction and electrostatic forces are the main acting forces. The molecular docking results manifest that AA interacts with the hydrophobic residues (Trp-571, Leu-568, Val-570 and Leu-576) and ionic interactions occur between Arg-579 and the -COOH of AA. The inhibitory activity of AA on HIV-1 JR-FL is quantified by 50% effective concentration (EC 50) and 90% effective concentration (EC 90), which are 31.42 ± 1.08 and 133.47 ± 18.10 μg mL−1, respectively. All the results indicate that AA is able to inhibit the formation of 6-HB but cannot disrupt the preformed 6-HB. Therefore, AA is a potential inhibitor for the viral fusion/entry. [ABSTRACT FROM AUTHOR]

Published

2018

5. Evaluation of sequence variability in HIV-1 gp41 C-peptide helix-grafted proteins.

Author

Tennyson, Rachel L., Walker, Susanne N., Ikeda, Terumasa, Harris, Reuben S., and McNaughton, Brian R.

Subjects

*C-peptide, *HIV, *VIRAL proteins, *PROTEIN-protein interactions, *PROTEIN folding, *PROTEIN engineering

Abstract

Many therapeutically-relevant protein-protein interactions (PPIs) have been reported that feature a helix and helix-binding cleft at the interface. Given this, different approaches to disrupting such PPIs have been developed. While short peptides (<15 amino acids) typically do not fold into a stable helix, researchers have reported chemical approaches to constraining helix structure. However, these approaches rely on laborious, and often expensive, chemical synthesis and purification. Our premise is that protein-based solutions that stabilize a therapeutically-relevant helix offer a number of advantages. In contrast to chemically constrained helical peptides, or minimal/miniature proteins, which must be synthesized (at great expense and labor), a protein can be expressed in a cellular system (like all current protein therapeutics). If selected properly, the protein scaffold can stabilize the therapeutically-relevant helix. We recently reported a protein engineering strategy, which we call “ helix-grafted display ”, and applied it to the challenge of suppressing HIV entry. We have reported helix-grafted display proteins that inhibit formation of an intramolecular PPI involving HIV gp41 C-peptide helix, and HIV gp41 N-peptide trimer, which contain C-peptide helix-binding clefts. Here, we used yeast display to screen a library of grafted C-peptide helices for N-peptide trimer recognition. Using ‘hits’ from yeast display library screening, we evaluated the effect helix mutations have on structure, expression, stability, function (target recognition), and suppression of HIV entry. [ABSTRACT FROM AUTHOR]

Published

2018

6. A novel peptide shows excellent anti-HIV-1 potency as a gp41 fusion inhibitor.

Author

Liu, Wei, An, Xiaohong, Wang, Jiao, Zhang, Xiaoguang, Tan, Jianjun, Zhou, Zhixiang, and Zeng, Yi

Subjects

*PEPTIDES, *ANTI-HIV agents, *VIRAL envelope proteins, *GENE rearrangement, *VIRAL replication, *ANTIRETROVIRAL agents

Abstract

Fusion inhibitors of HIV prevent the virus from entering into the target cell via the interaction with gp41, which stops the process of spatial rearrangement of the viral envelope protein. A series of peptides have been designed and screened to obtain a highly potent novel sequence. Among them, CT105 possesses the most potent anti-viral ability at low nanomolar IC50 values against a panel of HIV-1 pseudoviruses from A, B, C and A 1 /D subtypes, whereas T20 shows much weaker potency. CT105 also shows excellent inhibitory activity at 260 pico molar IC50 against HIV-1 replication. As a fusion inhibitor, CT105 has a strong ability to interrupt gp41 core formation. The terminal half-life of CT105 possesses 1.72-fold longer than that of T20 as determined by developing an indirect competitive ELISA method. The results suggest that this artificial peptide CT105 could be a favorable architype for further optimization and modification. [ABSTRACT FROM AUTHOR]

Published

2018

7. Synthesis and biological evaluation of water-soluble derivatives of chiral gossypol as HIV fusion inhibitors targeting gp41.

Author

Yang, Jian, Li, Long-Long, Li, Ju-Rong, Yang, Jing-Xiang, Zhang, Fang, Chen, Gang, Yu, Rui, Ouyang, Wen-Jie, and Wu, Shu-Wen

Subjects

*GOSSYPOL, *CHIRALITY, *HIV infections, *THERAPEUTICS, *GENE targeting, *GLUCOSAMINE derivatives

Abstract

A series of novel or known water-soluble derivatives of chiral gossypol were synthesized and screened in vitro for their anti-HIV-1 activity. (−)-gossypol derivative was more active against HIV-1 than the corresponding (+)-gossypol derivative, respectively. Among these derivatives, d -glucosamine derivative of (−)-gossypol, oligopeptide derivative of (−)-gossypol and taurine derivative of (−)-gossypol, such as compounds 1a , 3a and 14a , showed significant inhibitory activities against HIV-1 replication, HIV-1 mediated cell-cell fusion and HIV gp41 6-helix bundle formation as some amino acid derivatives of (−)-gossypol. [ABSTRACT FROM AUTHOR]

Published

2018

8. Structure-based identification of inhibitors targeting obstruction of the HIVgp41 N-heptad repeat trimer.

Author

Jr.McGee, T. Dwight, Yi, Hyun Ah, Allen, William J., Jacobs, Amy, and Rizzo, Robert C.

Subjects

*PROTEINS, *DRUGS, *CHEMICAL inhibitors, *CELLS, *CELL membranes

Abstract

The viral protein HIVgp41 is an attractive and validated drug target that proceeds through a sequence of conformational changes crucial for membrane fusion, which facilitates viral entry. Prior work has identified inhibitors that interfere with the formation of a required six-helix bundle, composed of trimeric C-heptad (CHR) and N -heptad (NHR) repeat elements, through blocking association of an outer CHR helix or obstructing formation of the inner NHR trimer itself. In this work, we employed similarity-based scoring to identify and experimentally characterize 113 compounds, related to 2 small-molecule inhibitors recently reported by Allen et al. ( Bioorg. Med. Chem Lett. 2015 , 25 2853–59), proposed to act via the NHR trimer obstruction mechanism. The compounds were first tested in an HIV cell-cell fusion assay with the most promising evaluated in a second, more biologically relevant viral entry assay. Of the candidates, compound #11 emerged as the most promising hit (IC 50 = 37.81 µM), as a result of exhibiting activity in both assays with low cytotoxicity, as was similarly seen with the known control peptide inhibitor C34. The compound also showed no inhibition of VSV-G pseudotyped HIV entry compared to a control inhibitor suggesting it was specific for HIVgp41. Molecular dynamics simulations showed the predicted DOCK pose of #11 interacts with HIVgp41 in an energetic fashion (per-residue footprints) similar to the four native NHR residues (IQLT) which candidate inhibitors were intended to mimic. [ABSTRACT FROM AUTHOR]

Published

2017

9. Development of a DNA vaccine expressing a secreted HIV-1 gp41 ectodomain that includes the membrane-proximal external region.

Author

Melnychuk, Luca, Ajamian, Lara, Jean-Pierre, Patrick, Liang, Jiaming, Gheorghe, Romina, Wainberg, Mark A., and Zaharatos, Gerasimos J.

Subjects

*DNA vaccines, *HIV, *POST-translational modification, *VACCINE manufacturing, *CHIMERIC proteins, *GENETIC mutation, *LABORATORY mice

Abstract

A limited number of sites on the HIV-1 Envelope protein are vulnerable to broadly neutralizing antibodies (bnAbs). One of these sites, the membrane proximal external region (MPER), is located at the C-terminus of the gp41 ectodomain (gp41 ecto ). This highly conserved sequence is bound by several well-characterized bnAbs. Efforts to produce a gp41 immunogen are in part hampered by the MPER’s hydrophobicity and propensity to induce aggregation. We sought to produce a DNA vaccine expressing a gp41 ecto that is both secreted from mammalian cells and maintains binding by bnAbs to the MPER. Through in silico analysis, we predicted regions of gp41 ecto that could induce aggregation and possibly hinder secretion. We generated deletion mutants of gp41 ecto and tested their ability to be secreted by mammalian cells. Upon deletion of regions in either the fusion peptide (FP) or MPER, secretion of the gp41 ecto increased. In an effort to both augment secretion and maintain binding by bnAbs, we developed constructs with the FP deletion and introduced point mutations in the MPER. Two constructs (gp41 ΔFP and gp41 ΔFP+I682E) maintained binding by gp41 MPER-specific bnAbs (4E10, Z13e1 and 10E8). These were evaluated as DNA vaccines in a mouse model. Both vaccines proved to be immunogenic and appeared to elicit some MPER-specific antibodies that bound gp41 ectodomain-derived proteins but not short peptides spanning the MPER. No neutralizing capacity was detected against a clade C virus containing a homologous MPER. [ABSTRACT FROM AUTHOR]

Published

2017

10. Multitargeted drug design strategy for discovery of short-peptide-based HIV-1 entry inhibitors with high potency.

Author

Wang, Chao, Wang, Huan, Wang, Xinling, Sun, Lujia, Wang, Qian, Li, Qing, Liang, Ruiying, Dou, Dou, Yu, Fei, Lu, Lu, and Jiang, Shibo

Subjects

*DRUG design, *HIV, *PEPTIDES, *CHEMOKINE receptors

Abstract

The development of short-peptide-based inhibitors to prevent HIV-1 entry into the host cell has been rewarded with limited success. Herein, we report a multitarget-directed ligand strategy to generate a series of short-peptide HIV-1 entry inhibitors that integrated the pharmacological activities of a peptide fusion inhibitor able to disrupt HIV-1 gp41 glycoprotein hexameric coiled-coil assembly and a small-molecule CCR5 antagonist that blocks the interaction between HIV-1 and its coreceptor. Among these inhibitors, dual-target 23-residue peptides SP12T and SP12L displayed dramatically increased inhibitory activities against HIV-1 replication as compared to the marketed 36-residue peptide T20. Moreover, results suggested that SP12T and SP12L successfully performed a dual-targeting mechanism. It can be concluded that these short-peptide-based HIV-1 entry inhibitors have potential for further development as candidates for a novel multitarget therapy to treat HIV-1 infection. [Display omitted] • Short peptide HIV entry inhibitors were designed via a multi-target design strategy. • Chimeras were obtained by linking together a CCR5 antagonist and a short-peptide SP22. • Dual-target inhibitors showed improved anti-HIV activity than parental inhibitors. • Dual-target short peptides had dramatically increased anti-HIV potency than T20. [ABSTRACT FROM AUTHOR]

Published

2023

11. A large HIV gp41 construct with trimer-of-hairpins structure exhibits V2E mutation-dominant attenuation of vesicle fusion and helicity very similar to V2E attenuation of HIV fusion and infection and supports: (1) hairpin stabilization of membrane apposition with larger distance for V2E; and (2) V2E dominance by an antiparallel β sheet with interleaved fusion peptide strands from two gp41 trimers

Author

Rokonujjaman, Md, Sahyouni, Abdulrazak, Wolfe, Robert, Jia, Lihui, Ghosh, Ujjayini, and Weliky, David P.

Subjects

*HIV infections, *C-terminal residues, *HIV, *PEPTIDES, *MEMBRANE separation, *VIRUS removal (Water purification)

Abstract

There is complete attenuation of fusion and infection mediated by HIV gp160 with gp41 subunit with V2E mutation, and also V2E dominance with WT/V2E mixtures. V2E is at the N-terminus of the ∼25-residue fusion peptide (Fp) which likely binds the target membrane. In this study, large V2E attenuation and dominance were observed for vesicle fusion induced by FP_HM, a large gp41 ectodomain construct with Fp followed by hyperthermostable hairpin with N- and C-helices, and membrane-proximal external region (Mper). FP_HM is a trimer-of-hairpins, the final gp41 structure during fusion. Vesicle fusion and helicity were measured for FP_HM using trimers with different fractions (f's) of WT and V2E proteins. Reductions in FP_HM fusion and helicity vs. f V2E were quantitatively-similar to those for gp160-mediated fusion and infection. Global fitting of all V2E data supports 6 WT gp41 (2 trimers) required for fusion. These data are understood by a model in which the ∼25 kcal/mol free energy for initial membrane apposition is compensated by the thermostable hairpin between the Fp in target membrane and Mper/transmembrane domain in virus membrane. The data support a structural model for V2E dominance with a membrane-bound Fp with antiparallel β sheet and interleaved strands from the two trimers. Relative to f V2E = 0, a longer Fp sheet is stabilized with small f V2E because of salt-bridge and/or hydrogen bonds between E2 on one strand and C-terminal Fp residues on adjacent strands, like R22. A longer Fp sheet results in shorter N- and C-helices, and larger separation during membrane apposition which hinders fusion. [Display omitted] • V2E is a dominant mutation for vesicle fusion by a large gp41 ectodomain construct. • V2E dominance is quantitatively-similar to that of gp160 fusion and HIV infectivity. • V2E-dominant reduction in helicity for the gp41 trimer-of-hairpins construct. • Final trimer-of-hairpins gp41 catalyzes initial membrane apposition step in fusion. • Two trimers required for efficient HIV fusion and infection. [ABSTRACT FROM AUTHOR]

Published

2023

12. Hybrids of small CD4 mimics and gp41-related peptides as dual-target HIV entry inhibitors.

Author

Wang, Rongyi, Tsuji, Kohei, Kobayakawa, Takuya, Liu, Yishan, Yoshimura, Kazuhisa, Matsushita, Shuzo, Harada, Shigeyoshi, and Tamamura, Hirokazu

Subjects

*CD4 antigen, *SMALL molecules, *PEPTIDES, *ANTI-HIV agents, *HIV, *MEMBRANE fusion

Abstract

[Display omitted] Hybrid molecules containing small CD4 mimics and gp41-C-terminal heptad repeat (CHR)-related peptides have been developed. A YIR-821 derivative was adopted as a CD4 mimic, which inhibits the interaction of gp120 with CD4. SC-peptides, SC34 and SC22EK, were also used as CHR-related peptides, which inhibit the interaction between the N -terminal heptad repeat (NHR) and CHR and thereby membrane fusion. Therefore, these hybrid molecules have dual-targets of gp120 and gp41. In the synthesis of the hybrid molecules of CD4 mimic-SC-peptides with different lengths of linkers, two conjugating methods, Cu-catalyzed azide-alkyne cycloaddition and direct cysteine alkylation, were performed. The latter reaction caused simpler operation procedures and higher synthetic yields than the former. The synthesized hybrid molecules of CD4 mimic-SC22EK have significantly higher anti-HIV activity than each sole agent. The present data should be useful in the future design of anti-HIV agents as dual-target entry inhibitors. [ABSTRACT FROM AUTHOR]

Published

2022

13. Screening HIV-1 fusion inhibitors based on capillary electrophoresis head-end microreactor targeting to the core structure of gp41.

Author

Liu, Lihong, Xu, Xiaoying, Liu, Yanhui, Zhang, Xuanxuan, Li, Lin, and Jia, Zhimin

Subjects

*HIV, *CAPILLARY electrophoresis, *ENZYME inhibitors, *MICROREACTORS, *MICROCHEMISTRY, *BUFFER solutions

Abstract

In this paper, we design a microreactor based on electrophoretically mediated microanalysis (EMMA) with capillary electrophoresis (CE) for screening HIV-1 inhibitors that bind to the N-terminal heptad repeat (NHR, N36) region. Initially, a test sample plug is loaded into a capillary filled with buffer solution followed by N36 peptide solution, and the two solutions simultaneously mix by diffusion. Then, voltage is applied, and the sample molecules pass through the N36 peptide zone. The active compounds combine with N36, leading to a loss in the peak height of the active compound. More than 100 traditional Chinese medicine extracts (TCME) were screened, and an extract of Pheretima aspergillum (E. Perrier) (L5) was identified as having potent inhibitory activity. The results showed that L5 could significantly inhibit the HIV-1 JR-FL pseudotyped virus infection; the 50% effective concentration (EC 50 ) of L5 was approximately 32.1 ± 1.2 μg/mL, and the 50% cytotoxicity concentration (CC 50 ) value of L5 was 146.9 ± 4.4 μg/mL, suggesting that L5 had low in vitro cytotoxicity on U87-CD4-CCR5 cells. The new method is simple and rapid, is free of antibodies, and does not require tedious processes. [ABSTRACT FROM AUTHOR]

Published

2016

14. Design, synthesis and activity evaluation of novel peptide fusion inhibitors targeting HIV-1 gp41.

Author

Tan, Jianjun, Su, Min, Zeng, Yi, and Wang, Cunxin

Subjects

*HIV, *HTLV, *PEPTIDES, *PROTEINS, *THANATOLOGY

Abstract

Human immunodeficiency virus type 1 (HIV-1), the pathogen of acquired immunodeficiency syndrome (AIDS), causes about 2 million people to death every year. Fusion inhibitors targeted the envelope protein (gp41) represent a novel and alternative approach for anti-AIDS therapy, which terminates the HIV-1 life cycle at an early stage. Using CP621-652 as a template, a series of peptides were designed, synthesized and evaluated in vitro assays. An interesting phenomenon was found that the substitution of hydrophobic residues at solvent accessible sites could increase the anti-HIV activity when the C-terminal sequence was extended with an enough numbers of amino acids. After the active peptides was synthesized and evaluated, peptide 8 showed the best anti-HIV-1 IIIB whole cell activity (MAGI IC 50 = 53.02 nM). Further study indicated that peptide 8 bound with the gp41 NHR helix, and then blocked the conformation of 6-helix, thus inhibited virus–cell membrane fusion. The results would be helpful for the design of peptide fusion inhibitors against HIV-1 infection. [ABSTRACT FROM AUTHOR]

Published

2016

15. Small molecule inhibitors of HIVgp41 N-heptad repeat trimer formation.

Author

Allen, William J., Yi, Hyun Ah, Gochin, Miriam, Jacobs, Amy, and Rizzo, Robert C.

Subjects

*SMALL molecules, *ANTI-HIV agents, *COMPUTER-assisted molecular design, *VIRAL proteins, *CHEMICAL inhibitors, *CELL fusion, *CELL-mediated cytotoxicity

Abstract

Identification of mechanistically novel anti-HIV fusion inhibitors was accomplished using a computer-aided structure-based design approach with the goal of blocking the formation of the N-heptad repeat (NHR) trimer of the viral protein gp41. A virtual screening strategy that included per-residue interaction patterns (footprints) was employed to identify small molecules compatible with putative binding pockets at the internal interface of the NHR helices at the core native viral six-helix bundle. From a screen of ∼2.8 million compounds using the DOCK program, 120 with favorable energetic and footprint overlap characteristics were purchased and experimentally tested leading to two compounds with favorable cell–cell fusion (IC 50 ) and cytotoxicity profiles. Importantly, both hits were identified on the basis of scores containing footprint overlap terms and would not have been identified using the standard DOCK energy function alone. To our knowledge, these compounds represent the first reported small molecules that inhibit viral entry via the proposed NHR-trimer obstruction mechanism. [ABSTRACT FROM AUTHOR]

Published

2015

16. Secondary structure assignment for conformationally irregular peptides: Comparison between DSSP, STRIDE and KAKSI.

Author

Zhang, Yuan and Sagui, Celeste

Subjects

*MOLECULAR structure, *PROTEIN conformation, *MOLECULAR dynamics, *PEPTIDES, *ASPARAGINE, *HYDROGEN bonding

Abstract

Secondary structure assignment codes were built to explore the regularities associated with the periodic motifs of proteins, such as those in backbone dihedral angles or in hydrogen bonds between backbone atoms. Precise structure assignment is challenging because real-life secondary structures are susceptible to bending, twist, fraying and other deformations that can distance them from their geometrical prototypes. Although results from codes such as DSSP and STRIDE converge in well-ordered structures, the agreement between the secondary structure assignments is known to deteriorate as the conformations become more distorted. Conformationally irregular peptides therefore offer a great opportunity to explore the differences between these codes. This is especially important for unfolded proteins and intrinsically disordered proteins, which are known to exhibit residual and/or transient secondary structure whose characterization is challenging. In this work, we have carried out Molecular Dynamics simulations of (relatively) disordered peptides, specifically gp41 659–671 (ELLELDKWASLWN), the homopeptide polyasparagine (N 18 ), and polyasparagine dimers. We have analyzed the resulting conformations with DSSP and STRIDE, based on hydrogen-bond patterns (and dihedral angles for STRIDE), and KAKSI, based on α -Carbon distances; and carefully characterized the differences in structural assignments. The full-sequence Segment Overlap (SOV) scores, that quantify the agreement between two secondary structure assignments, vary from 70% for gp41 659–671 (STRIDE as reference) to 49% for N 18 (DSSP as reference). Major differences are observed in turns, in the distinction between α and 3 10 helices, and in short parallel-sheet segments. [ABSTRACT FROM AUTHOR]

Published

2015

17. pH-dependent vesicle fusion induced by the ectodomain of the human immunodeficiency virus membrane fusion protein gp41: Two kinetically distinct processes and fully-membrane-associated gp41 with predominant β sheet fusion peptide conformation.

Author

Ratnayake, Punsisi U., Sackett, Kelly, Nethercott, Matthew J., and Weliky, David P.

Subjects

*PH effect, *HIV, *VIRAL envelopes, *MEMBRANE proteins, *HOSTS (Biology), *BIOLOGICAL membranes

Abstract

The gp41 protein of the Human Immunodeficiency Virus (HIV) catalyzes fusion between HIV and host cell membranes. The ~180-residue ectodomain of gp41 is outside the virion and is the most important gp41 region for membrane fusion. The ectodomain consists of an apolar fusion peptide (FP) region hypothesized to bind to the host cell membrane followed by N -heptad repeat (NHR), loop, and C -heptad repeat (CHR) regions. The present study focuses on the large gp41 ectodomain constructs “Hairpin” (HP) containing NHR + loop + CHR and “FP–Hairpin” (FP–HP) containing FP + NHR + loop + CHR. Both proteins induce rapid and extensive fusion of anionic vesicles at pH 4 where the protein is positively-charged but do not induce fusion at pH 7 where the protein is negatively charged. This observation, along with lack of fusion of neutral vesicles at either pH supports the significance of attractive protein/membrane electrostatics in fusion. There are two kinetically distinct fusion processes at pH 4: (1) a faster ~100 ms − 1 process with rate strongly positively correlated with vesicle charge; and (2) a slower ~5 ms − 1 process with extent strongly inversely correlated with this charge. The slower process may be more physiologically relevant because HIV/host cell fusion occurs at physiologic pH with gp41 restricted to the narrow region between the two membranes. Previous solid-state NMR (SSNMR) of membrane-associated FP–HP has supported protein oligomers with FP's in an intermolecular antiparallel sheet. There was an additional population of molecules with α helical FPs and the samples likely contained a mixture of membrane-bound and -unbound proteins. For the present study, samples were prepared with fully membrane-bound FP–HP and subsequent SSNMR showed dominant β FP conformation at both low and neutral pH. SSNMR also showed close contact of the FP with the lipid headgroups at both low and neutral pH whereas the NHR + CHR regions had contact at low pH and were more distant at neutral pH, consistent with the protein/membrane electrostatics. This article is part of a Special Issue entitled:NMR Spectroscopy for Atomistic Views of Biomembranes and Cell Surfaces. Guest Editors: Lynette Cegelski and David P. Weliky. [ABSTRACT FROM AUTHOR]

Published

2015

18. ADS-J1 inhibits HIV-1 infection and membrane fusion by targeting the highly conserved pocket in the gp41 NHR-trimer.

Author

Yu, Fei, Lu, Lu, Liu, Qi, Yu, Xiaowen, Wang, Lili, He, Elaine, Zou, Peng, Du, Lanying, Sanders, Rogier W., Liu, Shuwen, and Jiang, Shibo

Subjects

*HIV infections, *MEMBRANE fusion, *DRUG resistance, *GENETIC mutation, *MOLECULAR probes, *CIRCULAR dichroism

Abstract

Abstract: We previously identified a potent small-molecule human immunodeficiency virus type 1 (HIV-1) fusion inhibitor, termed ADS-J1, and hypothesized that it mainly targeted the hydrophobic pocket in the gp41 N-terminal heptad repeat (NHR) trimer. However, this hypothesis has been challenged by the fact that ADS-J1 cannot induce drug-resistance mutation in the gp41 pocket region. Therefore, we show herein that HIV-1 mutants resistant to T2635, a peptide derived from the gp41 C-terminal heptad repeat (CHR) region with pocket-binding domain (PBD), were also resistant to ADS-J1. We also show that pseudoviruses with mutations at positions 64 and 67 in the gp41 pocket region were highly resistant to ADS-J1 and C34, another CHR-peptide with PBD, but relatively sensitive to T20, a CHR-peptide without PBD. ADS-J1 could effectively bind to N36Fd, a mimic of the gp41 NHR-trimer with pocket exposed, and block binding of C34 to N36Fd trimer to form six-helix bundle (6-HB). However, ADS-J1 was less effective in binding to N36Fd trimer with mutations in the gp41 pocket region, such as N36(Q64A)Fd, N36(Q64L)Fd, N36(A67G)Fd, N36(A67S)Fd, and N36(Q66R)Fd, as well as less effective in blocking 6-HB formation between C34 and these mutant N36Fd trimers. These results confirm that ADS-J1 mainly targets the pocket region in the HIV-1 gp41 NHR trimer and suggest that it could be used as a lead for developing small-molecule HIV fusion inhibitors and as a molecule probe for studying the mechanisms of gp41-mediated membrane fusion. [Copyright &y& Elsevier]

Published

2014

19. Comparative mucosal immunogenicity of HIV gp41 membrane-proximal external region (MPER) containing single and multiple repeats of ELDKWA sequence with defensin peptides.

Author

Mohan, Teena, Verma, Priyanka, and Rao, D.N.

Subjects

*MUCOUS membranes, *IMMUNOGENETICS, *VIRAL proteins, *REPEATED sequence (Genetics), *DEFENSINS, *PEPTIDES, *HIV, *AIDS vaccines

Abstract

Abstract: The MPER of gp41 of HIV-1 has received great attention and is widely recognized as a promising target for the development of AIDS vaccine. We investigated the ability of trirepeat of ELDKWA sequence of gp41 antigen with defensins in liposome using multiple-shot immunization strategy in the mice model. The designed was used to enhance the immunogenicity and exposure of MPER in its native conformation for the induction of MPER-specific HIV-1 neutralizing antibodies. To characterize, we estimated the antibody levels (IgG/IgA) in serum as well as in lung, intestinal, vaginal and rectal washes till day 120 in outbred and inbred (H-2b and H-2d) mice using liposome as delivery vehicle. The representative sera and washes were also tested for in vitro neutralization with CCR5-tropic Indian HIV-1 primary isolates. We observed that the modified HIV antigen containing trirepeat of ELDKWA with defensins was showing significantly (p <0.001) higher IgG/IgA antibody titre (102,400–204,800) in sera as well as in different mucosal washes (1600–6400) than standard HIV-1 antigen. Furthermore, sera from the modified HIV-1 antigen with defensins found to exhibit higher neutralizing activities (ranging from 59.3% to 84.6%) than the standard HIV-1 antigen. These results show that the induction of MPER-specific HIV-1 neutralizing antibodies could be achieved through a rationally designed vaccine strategy. [Copyright &y& Elsevier]

Published

2014

20. Strategies for lead discovery: Application of footprint similarity targeting HIVgp41.

Author

Holden, Patrick M., Allen, William J., Gochin, Miriam, and Rizzo, Robert C.

Subjects

*TARGETED drug delivery, *VAN der Waals forces, *MOLECULAR dynamics, *GLYCOPROTEINS, *SOLVENTS, *PROTEIN-ligand interactions

Abstract

Abstract: A highly-conserved binding pocket on HIVgp41 is an important target for development of anti-viral inhibitors. Holden et al. (Bioorg. Med. Chem. Lett. 2012, 22, 3011) recently reported 7 experimentally-verified leads identified through a computational screen to the gp41 pocket in conjunction with a new DOCK scoring method (termed FPS scoring) developed in our laboratory. The method employs molecular footprints based on per-residue van der Waals interactions, electrostatic interactions, or the sum. In this work, we critically examine the gp41 screening results, prioritized using different scoring methods, in terms of two main criteria: (1) ligand pose properties which include footprint and energy score decompositions, MW, number of rotatable bonds, ligand efficiency, formal charge, and volume overlap, and (2) ligand pose stability which includes footprint stability (changes in footprint overlap) and rmsd stability (changes in geometry). Relative to standard DOCK scoring, pose property analyses demonstrate how FPS scoring can be used to identify ligands that mimic a known reference (derived here from the native gp41 substrate), while pose stability analyses demonstrate how FPS scoring can be used to enrich for compounds with greater overall stability during molecular dynamics (MD) simulations. Compellingly, of the 115 compounds tested experimentally, the 7 active compounds, as a group, more closely mimic the footprints made by the reference and show greater MD stability compared to the inactive group. Extensive studies using 116 protein–ligand complexes as controls reveal that ligands in their crystallographic binding pose also maintain higher FPS scores and smaller rmsds than do accompanying decoys, confirming that native poses are indeed ‘stable’ under the same conditions and that monitoring FPS variability during compound prioritization is likely to be beneficial. Overall, the results suggest the new scoring method will complement current virtual screening approaches for both the identification (FPS-ranking) and prioritization (FPS-stability) of target-compatible molecules in a quantitative and logical way. [Copyright &y& Elsevier]

Published

2014

21. F(ab′)2 fragment of a gp41 NHR-trimer-induced IgM monoclonal antibody neutralizes HIV-1 infection and blocks viral fusion by targeting the conserved gp41 pocket.

Author

Lu, Lu, Wei, Meili, Chen, Yanxia, Xiong, Weiliang, Yu, Fei, Qi, Zhi, Jiang, Shibo, and Pan, Chungen

Subjects

*IMMUNOGLOBULIN M, *MONOCLONAL antibodies, *VIRUSES, *IMMUNOTHERAPY, *CELL fusion, *BIOLOGICAL adaptation

Abstract

Abstract: Using a recombinant protein N46FdFc that mimics the HIV-1 gp41 N-helix trimer to immunize mice, we identified the first IgM monoclonal antibody 18D3 that specifically bound to the conserved gp41 pocket. Its F(ab′)2 fragment potently inhibited HIV-1 Env-mediated cell–cell fusion and neutralized infection by laboratory-adapted and primary HIV-1 isolates with different subtypes and tropism, including the T20-resistant variants. This F(ab′)2 fragment can be used to develop a bispecific broad neutralizing monoclonal antibody or HIV-1 inactivator as a novel immunotherapeutic for treatment and prevention of HIV-1 infection. [Copyright &y& Elsevier]

Published

2013

22. Identification of fragments targeting an alternative pocket on HIV-1 gp41 by NMR screening and similarity searching.

Author

Chu, Shidong and Gochin, Miriam

Subjects

*HIV, *GLYCOPROTEINS, *VIRAL proteins, *NUCLEAR magnetic resonance spectroscopy, *MEDICAL screening, *TARGETED drug delivery, *LIGANDS (Biochemistry)

Abstract

Abstract: The HIV-1 envelope glycoprotein gp41 fusion intermediate is a promising drug target for inhibiting viral entry. However, drug development has been impeded by challenges inherent in mediating the underlying protein–protein interaction. Here we report on the identification of fragments that bind to a C-terminal sub-pocket adjacent to the well-known hydrophobic pocket on the NHR coiled coil. Using a specifically designed assay and ligand-based NMR screening of a fragment library, we identified a thioenylaminopyrazole compound with a dissociation constant of ∼500μM. Interaction with the C-terminal sub-pocket was confirmed by paramagnetic relaxation enhancement NMR experiments, which also yielded the binding mode. Shape-based similarity searching detected additional phenylpyrazole and phenyltriazole fragments within the library, enriching the hit rate over random screening, and revealing molecular features required for activity. Discovery of the novel scaffolds and binding mechanism suggests avenues for extending the interaction surface and improving the potency of a hydrophobic pocket binding inhibitor. [Copyright &y& Elsevier]

Published

2013

23. Increase of anti-HIV activity of C-peptide fusion inhibitors using a bivalent drug design approach.

Author

Ling, Yanbo, Xue, Huifang, Jiang, Xifeng, Cai, Lifeng, and Liu, Keliang

Subjects

*ANTI-HIV agents, *C-peptide, *DRUG design, *N-terminal residues, *COMPARATIVE studies, *CHEMICAL templates

Abstract

Abstract: We reported the design of fusion inhibitors with improved activity using a multivalent inhibitor design strategy. First, we chose C29 as the template sequence, which is a 29-mer peptide derived from HIV-1 gp41 CHR domain and has anti-HIV activity of IC50 118nM in a cell–cell fusion assay. We optimized the crosslink sites and linkers of the template peptide. We found that N-terminal crosslink caused activity improvement based on the multivalent co-operative effect. Especially, the IC50 of peptide (CAcaC29)2 was improved from 49.02 (monomeric form) to 5.71nM. Compared with long peptides, short peptides may be more suitable to analyze the co-operative effect. So we selected a shorter peptide C22 to synthesize the bivalent inhibitors. Due its weak helicity, no co-operative effect appeared. Therefore, we chose SC22EK, which were introduced salt bridges to consolidate the helicity based on the natural sequence C22. The cross-linked (CAcaSC22EK)2 was four times more potent than the monomer SC22EK in anti-HIV activity, with an IC50 value of 4.92nM close to the high active peptide fusion inhibitor C34. The strategy used in this study may be used to design new fusion inhibitors to interfere similar processes. [Copyright &y& Elsevier]

Published

2013

24. Multimerized CHR-derived peptides as HIV-1 fusion inhibitors.

Author

Nomura, Wataru, Hashimoto, Chie, Suzuki, Takaharu, Ohashi, Nami, Fujino, Masayuki, Murakami, Tsutomu, Yamamoto, Naoki, and Tamamura, Hirokazu

Subjects

*PEPTIDES, *HIV, *ISOLEUCINE, *VIRAL proteins, *MONOMERS, *MEMBRANE fusion

Abstract

Abstract: To date, several HIV-1 fusion inhibitors based on the carboxy-terminal leucine/isoleucine heptad repeat (CHR) region of an HIV-1 envelope protein gp41 have been discovered. We have shown that a synthetic peptide mimetic of a trimer form of the CHR-derived peptide C34 has potent inhibitory activity against the HIV-1 fusion mechanism, compared to a monomer C34 peptide. The present study revealed that a dimeric form of C34 is evidently structurally critical for fusion inhibitors, and that the activity of multimerized CHR-derived peptides in fusion inhibition is affected by the properties of the unit peptides C34, SC34EK, and T20. The fluorescence-based study suggested that the N36-interactive sites of the C34 trimer, including hydrophobic residues, are exposed outside the trimer and that trimerization of C34 caused a remarkable increase in fusion inhibitory activity. The present results could be useful in the design of fusion inhibitors against viral infections which proceed via membrane fusion with host cells. [Copyright &y& Elsevier]

Published

2013

25. Addition of artificial salt bridge by Ile646Lys mutation in gp41 coiled-coil domain regulates 6-helical bundle formation.

Author

Zhao, Lei, Hu, Zhi-Wen, Tong, Pei, Chen, Yong-Xiang, Zhao, Yu-Fen, and Li, Yan-Mei

Subjects

*GENETIC mutation, *GENETIC regulation, *GLYCOPROTEINS, *INTERMEDIATES (Chemistry), *ENZYME inhibitors, *ANTIVIRAL agents, *CHOLESTEROL, *SUBSTITUTION reactions, *DRUG activation

Abstract

Abstract: HIV entry is mediated by the envelope glycoproteins gp120 and gp41. The gp41 subunit contains several functional domains: the N-terminal heptad repeat (NHR) domains fold a triple stranded coiled-coil forming a meta-stable prefusion intermediate. C-terminal heptad repeat (CHR) subsequently folds onto the hydrophobic grooves of the NHR coiled-coil to form a stable 6-helix bundle, which juxtaposes the viral and cellular membranes for fusion. The C34 which has 34 amino acid residues is known as the core structure in CHR. A highly anti-HIV peptide inhibitor derived from C34 was designed. An artificial salt bridge was added in the 6-helical bundle by substitution of lysine for Ile646. With a cholesterol modification at C-terminal, the inhibitor containing I646K mutation represented higher anti-viral activity than C34–cholesterol combination without mutation. [Copyright &y& Elsevier]

Published

2013

26. Mechanism of resistance to S138A substituted enfuvirtide and its application to peptide design

Author

Izumi, Kazuki, Kawaji, Kumi, Miyamoto, Fusasko, Shimane, Kazuki, Shimura, Kazuya, Sakagami, Yasuko, Hattori, Toshio, Watanabe, Kentaro, Oishi, Shinya, Fujii, Nobutaka, Matsuoka, Masao, Kaku, Mitsuo, Sarafianos, Stefan G., and Kodama, Eiichi N.

Subjects

*BIOCHEMICAL mechanism of action, *ENFUVIRTIDE (Drug), *DRUG design, *PEPTIDES, *DRUG resistance, *GENETIC mutation, *BINDING sites

Abstract

Abstract: T-20 (enfuvirtide) resistance is caused by the N43D primary resistance mutation at its presumed binding site at the N-terminal heptad repeat (N-HR) of gp41, accompanied by the S138A secondary mutation at the C-terminal HR of gp41 (C-HR). We have discovered that modifying T-20 to include S138A (T-20S138A) allows it to efficiently block wild-type and T20-resistant viruses, by a mechanism that involves improved binding of T-20S138A to the N-HR that contains the N43D primary mutation. To determine how HIV-1 in turn escapes T-20S138A we used a dose escalation method to select T-20S138A-resistant HIV-1 starting with either wild-type (HIV-1WT) or T-20-resistant (HIV-1N43D/S138A) virus. We found that when starting with WT background, I37N and L44M emerged in the N-HR of gp41, and N126K in the C-HR. However, when starting with HIV-1N43D/S138A, L33S and I69L emerged in N-HR, and E137K in C-HR. T-20S138A-resistant recombinant HIV-1 showed cross-resistance to other T-20 derivatives, but not to C34 derivatives, suggesting that T-20S138A suppressed HIV-1 replication by a similar mechanism to T-20. Furthermore, E137K enhanced viral replication kinetics and restored binding affinity with N-HR containing N43D, indicating that it acts as a secondary, compensatory mutation. We therefore introduced E137K into T-20S138A (T-20E137K/S138A) and revealed that T-20E137K/S138A moderately suppressed replication of T-20S138A-resistant HIV-1. T-20E137K/S138A retained activity to HIV-1 without L33S, which seems to be a key mutation for T-20 derivatives. Our data demonstrate that secondary mutations can be consistently used for the design of peptide inhibitors that block replication of HIV resistant to fusion inhibitors. [Copyright &y& Elsevier]

Published

2013

27. HIV-1 variants with a single-point mutation in the gp41 pocket region exhibiting different susceptibility to HIV fusion inhibitors with pocket- or membrane-binding domain

Author

Lu, Lu, Tong, Pei, Yu, Xiaowen, Pan, Chungen, Zou, Peng, Chen, Ying-Hua, and Jiang, Shibo

Subjects

*PROTEIN binding, *GENETIC mutation, *DISEASE susceptibility, *HIV fusion inhibitors, *ENFUVIRTIDE (Drug), *GENE targeting, *DRUG resistance

Abstract

Abstract: Enfuvirtide (T20), the first FDA-approved peptide HIV fusion/entry inhibitor derived from the HIV-1 gp41 C-terminal heptad-repeat (CHR) domain, is believed to share a target with C34, another well-characterized CHR-peptide, by interacting with the gp41 N-terminal heptad-repeat (NHR) to form six-helix bundle core. However, our previous studies showed that T20 mainly interacts with the N-terminal region of the NHR (N-NHR) and lipid membranes, while C34 mainly binds to the NHR C-terminal pocket region. But so far, no one has shown that C34 can induce drug-resistance mutation in the gp41 pocket region. In this study, we constructed pseudoviruses in which the Ala at the position of 67 in the gp41 pocket region was substituted with Asp, Gly or Ser, respectively, and found that these mutations rendered the viruses highly resistant to C34, but sensitive to T20. The NHR-peptide N36 with mutations of A67 exhibited reduced anti-HIV-1 activity and decreased α-helicity. The stability of six-helix bundle formed by C34 and N36 with A67 mutations was significantly lower than that formed by C34 and N36 with wild-type sequence. The combination of C34 and T20 resulted in potent synergistic anti-HIV-1 effect against the viruses with mutations in either N- or C-terminal region in NHR. These results suggest that C34 with a pocket-binding domain and T20 containing the N-NHR- and membrane-binding domains inhibit HIV-1 fusion by interacting with different target sites and the combinatorial use of C34 and T20 is expected to be effective against HIV-1 variants resistant to HIV fusion inhibitors. [Copyright &y& Elsevier]

Published

2012

28. Selected amino acid changes in HIV-1 subtype-C gp41 are associated with specific gp120V3 signatures in the regulation of co-receptor usage

Author

Dimonte, Salvatore, Babakir-Mina, Muhammed, Mercurio, Fabio, Di Pinto, Domenico, Ceccherini-Silberstein, Francesca, Svicher, Valentina, and Perno, Carlo-Federico

Subjects

*HIV, *VIRAL proteins, *AMINO acid sequence, *GLYCOPROTEINS, *ALGORITHMS, *PROTEIN analysis

Abstract

Abstract: The majority of studies have characterized the tropism of HIV-1 subtype-B isolates, but little is known about the determinants of tropism in other subtypes. So, the goal of the present study was to genetically characterize the envelope of viral proteins in terms of co-receptor usage by analyzing 356 full-length env sequences derived from HIV-1 subtype-C infected individuals. The co-receptor usage of V3 sequences was inferred by using the Geno2Pheno and PSSM algorithms, and also analyzed to the “11/25 rule”. All reported env sequences were also analyzed with regard to N-linked glycosylation sites, net charge and hydrophilicity, as well as the binomial correlation phi coefficient to assess covariation among gp120V3 and gp41 signatures and the average linkage hierarchical agglomerative clustering were also performed. Among env sequences present in Los Alamos Database, 255 and 101 sequences predicted as CCR5 and CXCR4 were selected, respectively. The classical V3 signatures at positions 11 and 25, and other specific V3 and gp41 amino acid changes were found statistically associated with different co-receptor usage. Furthermore, several statistically significant associations between V3 and gp41 signatures were also observed. The dendrogram topology showed a cluster associated with CCR5-usage composed by five gp41 mutated positions, A22V, R133M, E136G, N140L, and N166Q that clustered with T2VV3 and G24TV3 (bootstrap=1). Conversely, a heterogeneous cluster with CXCR4-usage, involving S11GRV3, 13–14insIG/LGV3, P16RQV3, Q18KRV3, F20ILVV3, D25KRQV3, Q32KRV3 along with A30Tgp41, S107Ngp41, D148Egp41, A189Sgp41 was identified (bootstrap=0.86). Our results show that as observed for HIV-1 subtype-B, also in subtype-C specific and different gp41 and gp120V3 amino acid changes are associated individually or together with CXCR4 and/or CCR5 usage. These findings strengthen previous observations that determinants of tropism may also reside in the gp41 protein. [Copyright &y& Elsevier]

Published

2012

29. Amino acid derivatives of the (−) enantiomer of gossypol are effective fusion inhibitors of human immunodeficiency virus type 1

Author

An, Tai, Ouyang, Wenjie, Pan, Wei, Guo, Deyin, Li, Jurong, Li, Longlong, Chen, Gang, Yang, Jian, Wu, Shuwen, and Tien, Po

Subjects

*AMINO acids, *ENANTIOMERS, *GOSSYPOL, *HIV, *MARAVIROC (Drug), *ANTIRETROVIRAL agents, *POLYPHENOLS, *CIRCULAR dichroism

Abstract

Abstract: T20 and maraviroc are the only two currently available entry inhibitors that have shown efficacy in treating HIV-1-infected individuals who have failed to respond to first-line antiretroviral drugs. Gossypol is a polyphenolic aldehyde extracted from cotton plants. By modifying the (−) enantiomer of gossypol with a series of small molecules, we have found that neutral amino acids with aliphatic group derivatives of (−) gossypol show the strongest inhibitory activity and the lowest cytotoxicity in vitro among all the derivatives tested. Additionally, the selectivity index of the (−) gossypol-neutral amino acid conjugates is increased 100-fold when compared with (−) gossypol alone. It is widely accepted that gossypol and gossypol derivatives inhibit HIV-1 replication by targeting reverse transcriptase. However, from the results of our time-of-addition assay, HIV-1-mediated cell fusion assay and VSV-G pseudotyped virus assay, we demonstrate that the alanine-(−) gossypol derivative ((−)G-Ala) is an effective HIV-1 entry inhibitor. Further mechanistic analysis revealed that (−)G-Ala neither blocks gp120-CD4 binding nor interacts with the HIV-1 co-receptor CXCR4. Results from sandwich ELISA, native-PAGE and circular dichroism (CD) show that (−)G-Ala inhibits the cell fusion-activated gp41 core domain. Moreover, (−)G-Ala binds to the HIV-5-Helix protein and blocking D-peptide (PIE7) binding to the hydrophobic pocket on the surface of the gp41 internal trimeric coiled-coil domain. The contraceptive properties of (−) gossypol and amino acid derivatives of (−) gossypol are also discussed. Collectively, our results indicate that (−)G-Ala may bind to the gp41 hydrophobic pocket and block the formation of the cell fusion-activated gp41 core to inhibit HIV-1-mediated membrane fusion and subsequent viral entry. [Copyright &y& Elsevier]

Published

2012

30. Induction of mucosal HIV-specific B and T cell responses after oral immunization with live coxsackievirus B4 recombinants

Author

Gu, Rui, Stagnar, Cristy, Zaichenko, Lesya, and Ramsingh, Arlene I.

Subjects

*COXSACKIEVIRUS diseases, *RECOMBINANT antibodies, *IMMUNIZATION, *B cells, *T cells, *ENTEROVIRUSES, *IMMUNE response, *PEPTIDES

Abstract

Abstract: Given the limited success of clinical HIV vaccine trials, new vaccine strategies are needed for the HIV pipeline. The present study explored the novel concept that a live enteric virus, with limited disease potential, is a suitable vaccine vector to elicit HIV-specific immune responses in the gut mucosa of immunized mice. Two coxsackievirus B4 (CVB4) vaccine vectors were designed to induce HIV-specific B or T cell responses. A B cell immunogen, CVB4/gp41(2F5), was constructed by expressing an epitope from the membrane proximal external region (MPER) of gp41 as a structural peptide within a surface loop of a capsid protein of CVB4. The T cell immunogen, CVB4/p24(733), was constructed previously by expressing a gag p24 sequence as a non-structural peptide at the amino-terminus of the CVB4 polyprotein. The CVB4/gp41(2F5) recombinant was antigenic in mice and elicited anti-gp41 antibodies in both the mucosal and systemic compartments. The route of immunization affected the antibody response since oral delivery of CVB4/gp41(2F5) induced anti-gp41 antibodies in the mucosal but not in the systemic compartment while parenteral delivery induced anti-gp41 antibodies in both compartments. In contrast, oral immunization with CVB4/p24(733) elicited both mucosal and systemic gag p24-specific T cell responses. Since coxsackieviruses are ubiquitous in the human population, a key question is whether pre-existing vector immunity will inhibit the ability of a CVB4-based vaccine to induce HIV-specific immune responses. We show that pre-existing vector immunity did not preclude the development of mucosal anti-gp41 antibodies or gag p24-specific T cell responses after oral immunization with the CVB4/HIV recombinants. We suggest that the CVB4/HIV recombinants have the potential to be a viable vaccine product because of ease of delivery, safety, immunogenicity, ease of large-scale production, and storage conditions requiring cold-chain temperatures provided by refrigeration. [Copyright &y& Elsevier]

Published

2012

31. Evaluation of a synthetic C34 trimer of HIV-1 gp41 as AIDS vaccines

Author

Hashimoto, Chie, Nomura, Wataru, Ohya, Aki, Urano, Emiko, Miyauchi, Kosuke, Narumi, Tetsuo, Aikawa, Haruo, Komano, Jun A., Yamamoto, Naoki, and Tamamura, Hirokazu

Subjects

*AIDS vaccines, *HIV, *VIRAL antigens, *BIOLOGICAL membranes, *GENE fusion, *IMMUNIZATION, *MOLECULAR structure

Abstract

Abstract: An artificial antigen forming the C34 trimeric structure targeting membrane-fusion mechanism of HIV-1 has been evaluated as an HIV vaccine. The C34 trimeric molecule was previously designed and synthesized using a novel template with C3-symmetric linkers by us. The antiserum produced by immunization of the C34 trimeric form antigen showed 23-fold higher binding affinity for the C34 trimer than for the C34 monomer and showed significant neutralizing activity. The present results suggest effective strategies of the design of HIV vaccines and anti-HIV agents based on the native structure mimic of proteins targeting dynamic supramolecular mechanisms in HIV fusion. [Copyright &y& Elsevier]

Published

2012

32. Discovery of HIV fusion inhibitors targeting gp41 using a comprehensive α-helix mimetic library

Author

Whitby, Landon R., Boyle, Kristopher E., Cai, Lifeng, Yu, Xiaoqian, Gochin, Miriam, and Boger, Dale L.

Subjects

*ANTIRETROVIRAL agents, *TARGETED drug delivery, *HIV, *BIOMOLECULES, *CELL fusion, *BIOLOGICAL assay

Abstract

Abstract: The evaluation of a comprehensive α-helix mimetic library for binding the gp41 NHR hydrophobic pocket recognizing an intramolecular CHR α-helix provided a detailed depiction of structural features required for binding and led to the discovery of small molecule inhibitors (K i 0.6–1.3μM) that not only match or exceed the potency of those disclosed over the past decade, but that also exhibit effective activity in a cell–cell fusion assay (IC50 5–8μM). [Copyright &y& Elsevier]

Published

2012

33. Molecular investigations into vaginal immunization with HIV gp41 antigenic construct H4A in a quick release solid dosage form

Author

Pattani, Aditya, McKay, Paul F., Curran, Rhonda M., McCaffrey, Joanne, Gupta, Prem N., Lowry, Deborah, Kett, Vicky L., Shattock, Robin J., McCarthy, Helen O., and Malcolm, R. Karl

Subjects

*VAGINAL medication, *IMMUNIZATION, *HIV, *SIMIAN immunodeficiency virus, *SOLID dosage forms, *IMMUNE response, *VACCINES, *INFECTIOUS disease transmission

Abstract

Abstract: A robust vaginal immune response is considered essential for an effective prophylactic vaccine that prevents transmission of HIV and other sexually acquired diseases. Considerable attention has recently focused on the potential of vaginally administered vaccines as a means to induce such local immunity. However, the potential for vaccination at this site remains in doubt as the vaginal mucosa is generally considered to have low immune inductive potential. In the current study, we explored for the first time the use of a quick release, freeze-dried, solid dosage system for practical vaginal administration of a protein antigen. These solid dosage forms overcome the common problem associated with leakage and poor retention of vaginally administered antigen solutions. Mice were immunized vaginally with H4A, an HIV gp41 envelope based recombinant protein, using quick release, freeze-dried solid rods, and the immune responses compared to a control group immunized via subcutaneous H4A injection. Vaginally immunized mice failed to elicit robust immune responses. Our detailed investigations, involving cytokine analysis, the stability of H4A in mouse cervicovaginal lavage, and elucidation of the state of H4A protein in the immediate-release dosage form, revealed that antigen instability in vaginal fluid, the state of the antigen in the dosage form, and the cytokine profile induced are all likely to have contributed to the observed lack of immunogenicity. These are important factors affecting vaginal immunization and provide a rational basis for explaining the typically poor and variable elicitation of immunity at this site, despite the presence of immune responsive cells within the vaginal mucosae. In future mucosal vaccine studies, a more explicit focus on antigen stability in the dosage form and the immune potential of available antigen-responsive cells is recommended. [Copyright &y& Elsevier]

Published

2012

34. Prime boost vaccination approaches with different conjugates of a new HIV-1 gp41 epitope encompassing the membrane proximal external region induce neutralizing antibodies in mice

Author

Zhou, Mingkui, Kostoula, Ioanna, Brill, Boris, Panou, Eugenia, Sakarellos-Daitsiotis, Maria, and Dietrich, Ursula

Subjects

*EPITOPES, *IMMUNOGLOBULINS, *HIV, *PEPTIDES, *MEMBRANE proteins, *BLOOD serum analysis, *VACCINATION, *LABORATORY mice

Abstract

Abstract: Peptide mimics of epitopes for pathogen-specific antibodies present in patient sera can be selected based on the phage display technology. Such mimotopes potentially represent vaccine candidates in case they are able to induce neutralizing antibodies upon vaccination. Here we analyze the immunogenicity of different conjugates of epitope EC26-2A4 localizing to the membrane proximal external region (MPER) of the HIV-1 transmembrane protein gp41. The EC26-2A4 epitope, which overlaps with that of the broadly neutralizing monoclonal antibody (mAb) 2F5, was coupled to sequential oligopeptide carriers (SOC) or to palmitoyl acid for better immunogenicity. Upon prime-boost immunizations of mice, the peptide conjugates induced EC26-2A4 specific antibodies in all settings and mice sera neutralized HIV-1SF162.LS in standardized neutralization assays. Thus, the EC26-2A4 MPER epitope represents a promising vaccine candidate for further analysis in larger animals with respect to the breadth of the neutralizing antibodies induced. [Copyright &y& Elsevier]

Published

2012

35. Compensatory mutations rescue the virus replicative capacity of VIRIP-resistant HIV-1

Author

González-Ortega, Emmanuel, Ballana, Ester, Badia, Roger, Clotet, Bonaventura, and Esté, José A.

Subjects

*HIV infections, *VIRAL replication, *GENETIC mutation, *ANTIRETROVIRAL agents, *DRUG resistance, *CELL culture, *AMINO acids, *SENSITIVITY analysis

Abstract

Abstract: VIRIP has been identified as a highly specific natural inhibitor of HIV-1 that blocks HIV-1 gp41-dependent fusion by interacting with the gp41 fusion peptide. Two analogues of VIRIP (VIR-353 and VIR-576) with a few amino acid changes increase its antiretroviral potency by two orders of magnitude in cell culture. VIR-576 has been shown effective in a phase I/II clinical trial. Resistance to VIRIP and its analogue VIR-353 were generated after long-term passage in cell culture suggesting a high genetic barrier to resistance. Mutations conferring resistance to VIRIP and VIR-353 significantly reduced virus fitness. However, accumulation of additional mutations rescued the replication capacity of the virus while retaining resistance to VIR-353 and full sensitivity to T20. Combinations of VIR-353 and T20 had an additive effect on the inhibition of wild type HIV-1 replication, but only a single agent was active when combinations were tested against T20-resistant HIV-1, suggesting that both gp41 peptides do not interfere with each other in their binding to gp41. Our results provide additional support to the development of a new class of antiretroviral agents targeting gp41-dependent fusion. [Copyright &y& Elsevier]

Published

2011

36. Design, synthesis, and biological activity of a novel series of 2,5-disubstituted furans/pyrroles as HIV-1 fusion inhibitors targeting gp41

Author

Jiang, Shibo, Tala, Srinivasa R., Lu, Hong, Zou, Peng, Avan, Ilker, Ibrahim, Tarek S., Abo-Dya, Nader E., Abdelmajeid, Abdelmotaal, Debnath, Asim K., and Katritzky, Alan R.

Subjects

*DRUG design, *HIV prevention, *ANTIVIRAL agents, *ORGANIC synthesis, *FURANS, *PYRROLES, *WITTIG reaction, *CELL fusion

Abstract

Abstract: Based on molecular docking analysis of earlier results, we designed a series of 2,5-disubstituted furans/pyrroles (5a–h) as HIV-1 entry inhibitors. Compounds were synthesized by Suzuki–Miyaura cross coupling, followed by a Knoevenagel condensation or Wittig reaction. Four of these compounds were found to be effective in inhibiting HIV-1 infection, with the best compounds being 5f and 5h, which exhibited significant inhibition on HIV-1IIIB infection at micromolar levels with low cytotoxicity. These compounds are also effective in blocking HIV-1 mediated cell-cell fusion and the gp41 six-helix bundle formation, suggesting that they are also HIV-1 fusion inhibitors targeting gp41 and have potential to be developed as a new class of anti-HIV-1 agents. [Copyright &y& Elsevier]

Published

2011

37. Viral surface glycoproteins, gp120 and gp41, as potential drug targets against HIV-1: Brief overview one quarter of a century past the approval of zidovudine, the first anti-retroviral drug

Author

Teixeira, Cátia, Gomes, José R.B., Gomes, Paula, and Maurel, François

Subjects

*HIV infections, *GLYCOPROTEINS, *DRUG target, *AZIDOTHYMIDINE, *ANTIRETROVIRAL agents, *DRUG development, *BIOACTIVE compounds

Abstract

Abstract: The first anti-HIV drug, zidovudine (AZT), was approved by the FDA a quarter of a century ago, in 1985. Currently, anti-HIV drug-combination therapies only target HIV-1 protease and reverse transcriptase. Unfortunately, most of these molecules present numerous shortcomings such as viral resistances and adverse effects. In addition, these drugs are involved in later stages of infection. Thus, it is necessary to develop new drugs that are able to block the first steps of viral life cycle. Entry of HIV-1 is mediated by its two envelope glycoproteins: gp120 and gp41. Upon gp120 binding to cellular receptors, gp41 undergoes a series of conformational changes from a non-fusogenic to a fusogenic conformation. The fusogenic core of gp41 is a trimer-of-hairpins structure in which three C-terminal helices pack against a central trimeric-coiled coil formed by three N-terminal helices. The formation of this fusogenic structure brings the viral and cellular membranes close together, a necessary condition for membrane fusion to occur. As gp120 and gp41 are attractive targets, the development of entry inhibitors represents an important avenue of anti-HIV drug therapy. The present review will focus on some general considerations about HIV, the main characteristics of gp120, gp41 and their inhibitors, with special emphasis on the advances of computational approaches employed in the development of bioactive compounds against HIV-1 entry process. [Copyright &y& Elsevier]

Published

2011

38. A mammalian two-hybrid system-based assay for small-molecular HIV fusion inhibitors targeting gp41

Author

Shui, Xiaoxi, Lu, Xinhua, Gao, Yan, Liu, Chen, Ren, Fengzhi, Jiang, Qin, Zhang, Hua, Zhao, Baohua, and Zheng, Zhihui

Subjects

*HIV fusion inhibitors, *GLYCOPROTEINS, *HIV, *FIRE assay, *VIRAL envelopes, *MEMBRANE fusion

Abstract

Abstract: gp41 is a major component of the envelope glycoprotein of human immunodeficiency virus type 1 (HIV-1) responsible for fusion of the viral envelope with the target cellular membrane. The formation of the trimer-of-hairpins core structure of gp41, via the interaction between its N-terminal heptad repeat (NHR) and its C-terminal heptad repeat (CHR) plays a key role in the membrane fusion process. Hence, inhibitors of trimer-of-hairpins formation have become a promising new class of HIV therapeutics. In the present study, based on the mammalian two-hybrid system, we developed a cell-based assay for detecting small-molecular HIV-1 fusion inhibitors targeting gp41. The optimized assay can be adapted to high-throughput screening in 96- and 384-well microplates with high signal-to-background ratios and acceptable Z′ factors. The known small-molecular gp41 inhibitors, ADS-J1, XTT formazan and tannin acid, tested positive in this assay, with half-maximal inhibitory concentration (IC50) values of 4.9μM, 5.6μM and 0.8μM, respectively. These data suggested that this novel assay is robust, sensitive and specific for identifying small-molecular HIV-1 gp41 inhibitors. [Copyright &y& Elsevier]

Published

2011

39. Characterization of HIV-1 resistance to a fusion inhibitor, N36, derived from the gp41 amino-terminal heptad repeat

Author

Izumi, Kazuki, Nakamura, Shota, Nakano, Hiroaki, Shimura, Kazuya, Sakagami, Yasuko, Oishi, Shinya, Uchiyama, Susumu, Ohkubo, Tadayasu, Kobayashi, Yuji, Fujii, Nobutaka, Matsuoka, Masao, and Kodama, Eiichi N.

Subjects

*HIV, *MEMBRANE fusion, *CELL fusion, *GLYCOPROTEINS, *ENZYME inhibitors, *PEPTIDES, *AMINO acids, *STABILITY (Mechanics)

Abstract

Abstract: A transmembrane glycoprotein of HIV-1, gp41, plays a central role in membrane fusion of HIV-1 and host cells. Peptides derived from the amino- and carboxyl-terminal heptad repeat (N-HR and C-HR, respectively) of gp41 inhibit this fusion. The mechanism of resistance to enfuvirtide, a C-HR-derived peptide, is well defined; however the mechanism of resistance to N-HR-derived peptides remains unclear. We characterized an HIV-1 isolate resistant to the N-HR-derived peptide, N36. This HIV-1 acquired a total of four amino acid substitutions, D36G, N126K and E137Q in gp41, and P183Q in gp120. Among these substitutions, N126K and/or E137Q conferred resistance to not only N36, but also C34, which is the corresponding C-HR-derived peptide fusion inhibitor. We performed crystallographic and biochemical analysis of the 6-helix bundle formed by synthetic gp41-derived peptides containing the N126K/E137Q substitutions. The structure of the 6-helix bundle with N126K/E137Q was identical to that in wild-type HIV-1 except for the presence of a new hydrogen bond. Denaturing experiments revealed that the stability of the 6-helix bundle of N126K/E137Q is greater than in the wild-type. These results suggest that the stabilizing effect of N126K/E137Q provides resistance to N36 and C34. [Copyright &y& Elsevier]

Published

2010

40. Kinetics of interaction of HIV fusion protein (gp41) with lipid membranes studied by real-time AFM imaging

Author

Bitler, Arkady, Lev, Naama, Fridmann-Sirkis, Yael, Blank, Lior, Cohen, Sidney R., and Shai, Yechiel

Subjects

*HIV, *VIRAL proteins, *HOST-virus relationships, *BILAYER lipid membranes, *ATOMIC force microscopy, *SURFACE roughness, *GLYCOPROTEINS, *PHOSPHATIDYLSERINES

Abstract

Abstract: One of the most important steps in the process of viral infection is a fusion between cell membrane and virus, which is mediated by the viral envelope glycoprotein. The study of activity of the glycoprotein in the post-fusion state is important for understanding the progression of infection. Here we present a first real-time kinetic study of the activity of gp41 (the viral envelope glycoprotein of human immunodeficiency virus—HIV) and its two mutants in the post-fusion state with nanometer resolution by atomic force microscopy (AFM). Tracking the changes in the phosphatidylcholine (PC) and phosphatidylcholine–phosphatidylserine (PC:PS) membrane integrity over one hour by a set of AFM images revealed differences in the interaction of the three types of protein with zwitterionic and negatively charged membranes. A quantitative analysis of the slow kinetics of hole formation in the negatively charged lipid bilayer is presented. Specifically, analysis of the rate of roughness change for the three types of proteins suggests that they exhibit different types of kinetic behavior. [Copyright &y& Elsevier]

Published

2010

41. Design, synthesis, and evaluation of indole compounds as novel inhibitors targeting Gp41

Author

Zhou, Guangyan, Wu, Dong, Hermel, Evan, Balogh, Edina, and Gochin, Miriam

Subjects

*INDOLE, *ORGANIC synthesis, *CHEMICAL inhibitors, *GLYCOPROTEINS, *LIGAND binding (Biochemistry), *CELL communication, *BIOLOGICAL assay, *LEAD compounds

Abstract

Abstract: A series of indole ring containing compounds were designed based on the structure of the gp41 complex in the region of the hydrophobic pocket. These compounds were synthesized using a Suzuki Coupling reaction, and evaluated using a fluorescence binding assay and cell–cell fusion assay. The observed inhibition constant of compound 7 was 2.1μM, and the IC50 for cell–cell fusion inhibition was 1.1μM. Assay data indicated that 7 is a promising lead compound for optimization into an effective low molecular weight fusion inhibitor. [Copyright &y& Elsevier]

Published

2010

42. HIV-1 gp41 fusion intermediate: a target for HIV therapeutics.

Author

Pan, Chungen, Liu, Shuwen, and Jiang, Shibo

Subjects

HIV infections, THERAPEUTICS, GLYCOPROTEINS, CELL receptors, MEMBRANE proteins, VIRAL envelopes, PEPTIDES, ANTIVIRAL agents, COMPARATIVE studies, HIV, RESEARCH methodology, MEDICAL cooperation, RESEARCH, VIRAL antigens, DRUG development, EVALUATION research, ANTI-HIV agents, PHARMACODYNAMICS, CELL physiology

Abstract

Human immunodeficiency virus (HIV)-1 infection is initiated by the binding of gp120 envelope glyco-protein to its cell receptor (CD4) and a coreceptor (CXCR4 or CCR5), followed by a series of conformational changes in the gp41 transmembrane subunit. These changes include insertion of fusion peptide into the target cell membrane and association of C-heptad repeat (CHR) peptide with the N-heptad repeat (NHR) trimer, a pre-hairpin fusion intermediate. A stable six-helix bundle core is then formed, bringing the viral envelope and target cell membrane into close proximity for fusion. Peptides derived from the CHR region, such as T20 and C34, inhibit HIV-1 fusion by interacting with the gp41 fusion intermediate. A number of anti-HIV-1 peptides and small molecule compounds targeting the gp41 NHR-trimer have been identified. By combining HIV fusion/entry inhibitors targeting different sites in the gp41 fusion intermediate, a potent synergistic effect takes place, resulting in a potential new therapeutic strategy for the HIV infection/AIDS. Here, we present an overview of the current development of anti-HIV drugs, particularly those targeting the gp41 fusion intermediate. [Copyright &y& Elsevier]

Published

2010

43. Non-peptide entry inhibitors of HIV-1 that target the gp41 coiled coil pocket

Author

Stewart, Kent D., Huth, Jeffrey R., Ng, Teresa I., McDaniel, Keith, Hutchinson, Rebecca Newlin, Stoll, Vincent S., Mendoza, Renaldo R., Matayoshi, Edmund D., Carrick, Robert, Mo, HongMei, Severin, Jean, Walter, Karl, Richardson, Paul L., Barrett, Leo W., Meadows, Robert, Anderson, Steve, Kohlbrenner, William, Maring, Clarence, Kempf, Dale J., and Molla, Akhter

Subjects

*PEPTIDE drugs, *HIV infections, *THERAPEUTICS, *CELL membranes, *VIRAL proteins, *BENZAMIDE, *CELL fusion, *NUCLEAR magnetic resonance spectroscopy, *HOST-virus relationships

Abstract

Abstract: The ectodomain of HIV-1 gp41 mediates the fusion of viral and host cellular membranes. The peptide-based drug Enfuvirtide is precedent that antagonists of this fusion activity may act as anti HIV-agents. Here, NMR screening was used to discover non-peptide leads against this target and resulted in the discovery of a new benzamide 1 series. This series is non-peptide, low molecular weight, and analogs have activity in a cell fusion assay with EC50 values ranging 3–41μM. Structural work on the gp41/benzamide 1 complex was determined by NMR spectroscopy using a designed model peptide system that mimics an open pocket of the fusogenic form of the protein. [Copyright &y& Elsevier]

Published

2010

44. Structure-based design, synthesis and biological evaluation of new N-carboxyphenylpyrrole derivatives as HIV fusion inhibitors targeting gp41

Author

Wang, Yong, Lu, Hong, Zhu, Qiang, Jiang, Shibo, and Liao, Yun

Subjects

*PYRROLES, *LIGANDS (Biochemistry), *DRUG design, *GLYCOPROTEINS, *X-ray crystallography, *ANTIVIRAL agents, *HIV, *VIRAL replication

Abstract

Abstract: A new series of N-carboxyphenylpyrrole ligands were designed using GeometryFit based on an X-ray crystal structure of gp41. The synthesized ligands showed significant inhibitory activities against HIV gp41 6-helix bundle formation, HIV-1 mediated cell–cell fusion and HIV-1 replication. [Copyright &y& Elsevier]

Published

2010

45. Structure-based design of substituted biphenyl ethylene ethers as ligands binding in the hydrophobic pocket of gp41 and blocking the helical bundle formation

Author

Liu, Bin, Joseph, Rhoda W., Dorsey, Bruce D., Schiksnis, Robert A., Northrop, Katrina, Bukhtiyarova, Marina, and Springman, Eric B.

Subjects

*ETHERS, *ETHYLENE, *SUBSTITUTION reactions, *MOLECULAR structure, *LIGAND binding (Biochemistry), *GLYCOPROTEINS, *HIGH performance liquid chromatography, *BIOLOGICAL assay

Abstract

Abstract: A series of substituted biphenyl ethylene ether compounds has been designed to target the gp41N-trimer in order to inhibit formation of the six-helical bundle that represents the end state of gp41-mediated viral fusion. A size exclusion HPLC based helical bundle formation (HBF) assay was developed to evaluate in vitro inhibitory affinity of the inhibitors. The most potent compound 1 had an IC50 of 31μM. The binding of compound 1 to the proposed hydrophobic pocket of gp41 was further validated by site-directed peptide mutagenesis experiments. [Copyright &y& Elsevier]

Published

2009

46. Membrane topology of gp41 and amyloid precursor protein: Interfering transmembrane interactions as potential targets for HIV and Alzheimer treatment

Author

Abad, Concepción, Martínez-Gil, Luis, Tamborero, Silvia, and Mingarro, Ismael

Subjects

*BIOLOGICAL membranes, *GLYCOPROTEINS, *AMYLOID beta-protein precursor, *PROTEIN-protein interactions, *ALZHEIMER'S disease treatment, *HIV infections, *THERAPEUTICS, *PROTEIN structure, *AMINO acid sequence, *TARGETED drug delivery

Abstract

Abstract: The amyloid precursor protein (APP), that plays a critical role in the development of senile plaques in Alzheimer disease (AD), and the gp41 envelope protein of the human immunodeficiency virus (HIV), the causative agent of the acquired immunodeficiency syndrome (AIDS), are single-spanning type-1 transmembrane (TM) glycoproteins with the ability to form homo-oligomers. In this review we describe similarities, both in structural terms and sequence determinants of their TM and juxtamembrane regions. The TM domains are essential not only for anchoring the proteins in membranes but also have functional roles. Both TM segments contain GxxxG motifs that drive TM associations within the lipid bilayer. They also each possess similar sequence motifs, positioned at the membrane interface preceding their TM domains. These domains are known as cholesterol recognition/interaction amino acid consensus (CRAC) motif in gp41 and CRAC-like motif in APP. Moreover, in the cytoplasmic domain of both proteins other α-helical membranotropic regions with functional implications have been identified. Recent drug developments targeting both diseases are reviewed and the potential use of TM interaction modulators as therapeutic targets is discussed. [Copyright &y& Elsevier]

Published

2009

47. Molecular dynamics studies of the transmembrane domain of gp41 from HIV-1

Author

Kim, Jong Hwa, Hartley, Taryn L., Curran, A. Rachael, and Engelman, Donald M.

Subjects

*MOLECULAR dynamics, *MEMBRANE proteins, *HIV, *MOLECULE-molecule collisions, *GLYCOPROTEINS, *CONFORMATIONAL analysis, *BILAYER lipid membranes, *ARGININE

Abstract

Abstract: Helix–helix interactions in the putative three-helix bundle formation of the gp41 transmembrane (TM) domain may contribute to the process of virus–cell membrane fusion in HIV-1 infection. In this study, molecular dynamics is used to analyze and compare the conformations of monomeric and trimeric forms of the TM domain in various solvent systems over the course of 4 to 23-ns simulations. The trimeric bundles of the TM domain were stable as helices and remained associated in a hydrated POPE lipid bilayer for the duration of the 23-ns simulation. Several stable inter-chain hydrogen bonds, mostly among the three deprotonated arginine residues located at the center of each of the three TM domains, formed in a right-handed bundle embedded in the lipid bilayer. No such bonds were observed when the bundle was left-handed or when the central arginine residue in each of the three TM helices was replaced with isoleucine (R_I mutant), suggesting that the central arginine residues may play an essential role in maintaining the integrity of the three-helix bundle. These observations suggest that formation of the three-helix bundle of the TM domain may play a role in the trimerization of gp41, thought to occur during the virus–cell membrane fusion process. [Copyright &y& Elsevier]

Published

2009

48. Synonymous mutations in stem-loop III of Rev responsive elements enhance HIV-1 replication impaired by primary mutations for resistance to enfuvirtide

Author

Ueno, Mariko, Kodama, Eiichi N., Shimura, Kazuya, Sakurai, Yasuteru, Kajiwara, Keiko, Sakagami, Yasuko, Oishi, Shinya, Fujii, Nobutaka, and Matsuoka, Masao

Subjects

*HIV, *GENETIC mutation, *NUCLEOTIDES, *VIRAL replication

Abstract

Abstract: Primary mutations in HIV-1 that are directly involved in the resistance to enfuvirtide have been well documented. However, secondary mutations that are associated with primary mutations and contribute little to the resistance still remain to be elucidated. This study reveals that synonymous mutations at gp41 Q41 (CAG to CAA) or L44 (UUG to CUG) act as secondary mutations. Complementary mutations in the nucleotide level are located in the Rev responsive element (RRE) of the HIV-1 RNA-genome and maintain the replication kinetics of HIV-1 through increasing the structural stability of stem-loop III in the RRE. Therefore, synonymous mutations in the gp41/RRE sequence improve the viral replication impaired by the primary mutations and play a key role as secondary (complementary) mutations. [Copyright &y& Elsevier]

Published

2009

49. Cross-reactive HIV-1-neutralizing activity of serum IgG from a rabbit immunized with gp41 fused to IgG1 Fc: Possible role of the prolonged half-life of the immunogen

Author

Zhang, Mei-Yun, Wang, Yanping, Mankowski, Marie K., Ptak, Roger G., and Dimitrov, Dimiter S.

Subjects

*AIDS prevention, *AIDS vaccines, *IMMUNOGLOBULIN G, *HIV antibodies, *ANTIGEN-antibody reactions, *IMMUNOGENETICS, *LABORATORY rabbits, *EPITOPES, *MEDICAL research

Abstract

Abstract: The elicitation of broadly cross-reactive HIV-1 neutralizing antibodies in humans remains a major challenge in developing a viable AIDS vaccine. We hypothesized that prolonged exposure to candidate vaccine immunogens could enhance the elicitation of such antibodies. In an attempt to develop HIV-1 vaccine immunogens with prolonged half-lives and increased stability, we constructed a fusion protein, gp41Fc, in which a truncated HIV-1 gp4189.6 was fused to a human IgG1 Fc. Gp41Fc is stable in solution, retains its antigenic structure and is highly immunogenic in rabbits. The serum titers reached 1:102,400 for the gp41Fc and 1:5,120 for gp14089.6. Rabbit IgG neutralized diverse HIV-1 isolates and HIV-2, and the neutralization activity was attributed to gp41-specific IgG. The concentration of the gp41Fc in the serum correlated with the neutralization activity of rabbit IgG which recognized mostly conformation-independent epitopes on gp41 and predominantly bound to peptides derived from the gp41 immunodominant loop region. These results suggest that the prolonged half-life of gp41Fc in the serum may enhance the generation of cross-reactive neutralizing antibodies. Further research is needed to confirm and extend these results which may have implications for the development of vaccine immunogens with enhanced capability to elicit cross-reactive HIV-1-neutralizing antibodies. [Copyright &y& Elsevier]

Published

2009

50. The SARS CoV-2 spike directed non-neutralizing polyclonal antibodies cross-react with Human immunodeficiency virus (HIV-1) gp41.

Author

Perween, Reshma, PraveenKumar, Murugavelu, Shrivastava, Tripti, Parray, Hilal Ahmed, Singh, Vanshika, Singh, Swarandeep, Chiranjivi, Adarsh, Jakhar, Kamini, Sonar, Sudipta, Tiwari, Mahima, Reema, Panchal, Anil Kumar, Sharma, Chandresh, Rathore, Deepak Kumar, Ahamed, Shubbir, Samal, Sweety, Mani, Shailendra, Bhattacharyya, Sankar, Das, Supratik, and Luthra, Kalpana

Subjects

*HIV antibodies, *SARS-CoV-2, *VIRUS diseases, *RNA viruses, *ANTIBODY formation, *HIV

Abstract

• Cross talk between SARS CoV-2 and HIV-1. • Non-neutralizing antibody cross reactivity response connecting SARS CoV-2 and HIV-1. • Cross reactive responses among different class I viruses. • Non-neutralizing antibody responses can contribute towards ADCC mediated protection. Cross-reactivity among the two diverse viruses is believed to originate from the concept of antibodies recognizing similar epitopes on the two viral surfaces. Cross-reactive antibody responses have been seen in previous variants of SARS and SARS-CoV-2, but little is known about the cross reactivity with other similar RNA viruses like HIV-1. In the present study, we examined the reactivity the SARS-CoV-2 directed antibodies, via spike, immunized mice sera and demonstrated whether they conferred any cross-reactive neutralization against HIV-1. Our findings show that SARS-CoV-2 spike immunized mice antibodies cross-react with the HIV-1 Env protein. Cross-neutralization among the two viruses is uncommon, suggesting the presence of a non-neutralizing antibody response to conserved epitopes amongst the two viruses. Our results indicate, that SARS-CoV-2 spike antibody cross reactivity is targeted towards the gp41 region of the HIV-1 Env (gp160) protein. Overall, our investigation not only answers a crucial question about the understanding of cross-reactive epitopes of antibodies generated in different viral infections, but also provides critical evidence for developing vaccine immunogens and novel treatment strategies with enhanced efficacy capable of recognising diverse pathogens with similar antigenic features. [ABSTRACT FROM AUTHOR]

Published

2021