Discovery of Novel Small-Molecule Inhibitors of LIM Domain Kinase for Inhibiting HIV-1

ABSTRACT A dynamic actin cytoskeleton is necessary for viral entry, intracellular migration, and virion release. For HIV-1 infection, during entry, the virus triggers early actin activity by hijacking chemokine coreceptor signaling, which activates a host dependency factor, cofilin, and its kinase, the LIM domain kinase (LIMK). Although knockdown of human LIM domain kinase 1 (LIMK1) with short hairpin RNA (shRNA) inhibits HIV infection, no specific small-molecule inhibitor of LIMK has been available. Here, we describe the design and discovery of novel classes of small-molecule inhibitors of LIMK for inhibiting HIV infection. We identified R10015 as a lead compound that blocks LIMK activity by binding to the ATP-binding pocket. R10015 specifically blocks viral DNA synthesis, nuclear migration, and virion release. In addition, R10015 inhibits multiple viruses, including Zaire ebolavirus (EBOV), Rift Valley fever virus (RVFV), Venezuelan equine encephalitis virus (VEEV), and herpes simplex virus 1 (HSV-1), suggesting that LIMK inhibitors could be developed as a new class of broad-spectrum antiviral drugs. IMPORTANCE The actin cytoskeleton is a structure that gives the cell shape and the ability to migrate. Viruses frequently rely on actin dynamics for entry and intracellular migration. In cells, actin dynamics are regulated by kinases, such as the LIM domain kinase (LIMK), which regulates actin activity through phosphorylation of cofilin, an actin-depolymerizing factor. Recent studies have found that LIMK/cofilin are targeted by viruses such as HIV-1 for propelling viral intracellular migration. Although inhibiting LIMK1 expression blocks HIV-1 infection, no highly specific LIMK inhibitor is available. This study describes the design, medicinal synthesis, and discovery of small-molecule LIMK inhibitors for blocking HIV-1 and several other viruses and emphasizes the feasibility of developing LIMK inhibitors as broad-spectrum antiviral drugs.

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Diverse Effects of Small Molecule Inhibitors on Actin Cytoskeleton Dynamics in HIV-1 Infection

Journal of Bacteriology and Virology ◽

10.4167/jbv.2019.49.2.69 ◽

2019 ◽

Vol 49 (2) ◽

pp. 69

Author(s):

YoungHyun Shin ◽

Byeong-Sun Choi ◽

Kyung-Chang Kim ◽

Kisoon Kim ◽

Cheol-Hee Yoon

Keyword(s):

Actin Cytoskeleton ◽

Small Molecule ◽

Small Molecule Inhibitors ◽

Cytoskeleton Dynamics ◽

Hiv 1

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Interaction of small molecule inhibitors of HIV-1 entry with CCR5

Virology ◽

10.1016/j.virol.2006.01.018 ◽

2006 ◽

Vol 349 (1) ◽

pp. 41-54 ◽

Cited By ~ 98

Author(s):

Christoph Seibert ◽

Weiwen Ying ◽

Svetlana Gavrilov ◽

Fotini Tsamis ◽

Shawn E. Kuhmann ◽

...

Keyword(s):

Small Molecule ◽

Small Molecule Inhibitors ◽

Hiv 1

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Small-Molecule Inhibitors of HIV-1 Protease Dimerization Derived from Cross-Linked Interfacial Peptides

Angewandte Chemie ◽

10.1002/1521-3757(20000804)112:15<2822::aid-ange2822>3.0.co;2-1 ◽

2000 ◽

Vol 112 (15) ◽

pp. 2822-2825 ◽

Cited By ~ 4

Author(s):

Michael D. Shultz ◽

Michael J. Bowman ◽

Young-Wan Ham ◽

Xuimin Zhao ◽

George Tora ◽

...

Keyword(s):

Small Molecule ◽

Small Molecule Inhibitors ◽

Hiv 1

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Release of gp120 Restraints Leads to an Entry-Competent Intermediate State of the HIV-1 Envelope Glycoproteins

mBio ◽

10.1128/mbio.01598-16 ◽

2016 ◽

Vol 7 (5) ◽

Cited By ~ 59

Author(s):

Alon Herschhorn ◽

Xiaochu Ma ◽

Christopher Gu ◽

John D. Ventura ◽

Luis Castillo-Menendez ◽

...

Keyword(s):

Small Molecule ◽

Intermediate State ◽

Neutralizing Antibodies ◽

Small Molecule Inhibitors ◽

Virus Entry ◽

Envelope Glycoproteins ◽

Low Levels ◽

State 1 ◽

Hiv 1 ◽

Conformation State

ABSTRACTPrimary human immunodeficiency virus (HIV-1) envelope glycoprotein (Env) trimers [(gp120/gp41)3] typically exist in a metastable closed conformation (state 1). Binding the CD4 receptor triggers Env to undergo extensive conformational changes to mediate virus entry. We identified specific gp120 residues that restrain Env in state 1. Alteration of these restraining residues destabilized state 1, allowing Env to populate a functional conformation (state 2) intermediate between state 1 and the full CD4-bound state (state 3). Increased state 2 occupancy was associated with lower energy barriers between the states. State 2 was an obligate intermediate for all transitions between state 1 and state 3. State 2-enriched Envs required lower CD4 concentrations to trigger virus entry and more efficiently infected cells expressing low levels of CD4. These Envs were resistant to several broadly neutralizing antibodies and small-molecule inhibitors. Thus, state 2 is an Env conformation on the virus entry pathway; sampling state 2 increases the adaptability of HIV-1 to different host cell receptor levels and immune environments. Our results provide new insights into the conformational regulation of HIV-1 entry.IMPORTANCEThe envelope glycoproteins (Env) of HIV-1 mediate virus entry and are the sole targets of neutralizing antibodies. Understanding the way that Env promotes HIV-1 entry can expedite drug and vaccine development. By destabilizing Env, we found that it assumes an intermediate state that is functional and obligate for transitions to entry-competent conformations. Increased sampling of this state enhances the ability of HIV-1 to infect cells that express low levels of the CD4 receptor and allows the virus to evade neutralizing antibodies and small-molecule inhibitors. These findings provide new mechanistic insights into the function and inhibition of HIV-1 Env and will contribute to ongoing therapeutic and prevention efforts to combat HIV-1.

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