GroEL/ES inhibitors as potential antibiotics

Abdeen, Sanofar; Salim, Nilshad; Mammadova, Najiba; Summers, Corey M.; Frankson, Rochelle; Ambrose, Andrew J.; Anderson, Gregory G.; Schultz, Peter G.; Horwich, Arthur L.; Chapman, Eli; Johnson, Steven M.

doi:10.1016/j.bmcl.2016.04.089

Cited by 35 publications

(67 citation statements)

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“…Sequencing of Hsp65 genes within a family of mycobacteria can be used for sub-classification of mycobacterial species [3][4][5]. In bacterial species, Hsp65 is known as GroEL, and the human homologue is known as human Hsp60, with similar molecular functions in both bacterial and human cells [6,7]. Previous studies demonstrated the presence of anti-Hsp65 antibodies within the circulation of patients with a variety of chronic conditions, including autoimmune diseases such as multiple sclerosis (MS), systemic lupus erythematosus (SLE), and Crohn's disease (CD), as well as other chronic conditions such as heart disease, atherosclerosis, and different types of cancers [8][9][10][11].…”

Section: Introductionmentioning

confidence: 99%

Serological Testing for Mycobacterial Heat Shock Protein Hsp65 Antibody in Health and Diseases

Zhang¹,

Minardi²,

Kuenstner³

et al. 2019

Microorganisms

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Mycobacterial heat shock protein 65 gene (Hsp65) has been widely used for classification of Mycobacterial species, and detection of Mycobacterial genes by molecular methods and has proven useful in identification of Mycobacterial infection in various clinical conditions. Circulating antibody against Mycobacterial hsp65 has been found in many clinical diseases including autoimmune diseases (Crohn’s disease, lupus erythematosus, multiple sclerosis, diabetes, etc.), atherosclerosis and cancers. The prevalence of anti-Hsp65 antibody in the normal healthy population is unknown. We determined the blood levels of antibody against Mycobacterial hsp65 in the normal population represented by 288 blood donors of the American Red Cross and tested the blood of 109 patients with Crohn’s disease and 28 patients with Sjogren’s syndrome for comparison. The seroprevalence of anti-Hsp65 IgG in the normal population of Red Cross donors was 2.8% (8 of 288 positive). The Hsp65 antibody levels were significantly elevated in patients with Crohn’s disease and Sjogren’s syndrome. The prevalence of Hsp65 antibody in Crohn’s disease patients was 67.9% (74 of 109 patients), and 85.7% for Sjogren’s patients (24 of 28 patients). Our data indicate that anti-Hsp65 antibody is rare in the normal population, but frequent in chronic diseases. The presence of circulating Hsp65 antibody reflects an abnormal immune (adaptive) response to Mycobacterial exposure in patients with chronic diseases, thus differentiating the patients with chronic diseases from those clinical mimics.

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Section: Introductionmentioning

confidence: 99%

Serological Testing for Mycobacterial Heat Shock Protein Hsp65 Antibody in Health and Diseases

Zhang¹,

Minardi²,

Kuenstner³

et al. 2019

Microorganisms

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“…33 We have since found that several of our chaperonin inhibitors exhibit antibiotic effects against Gram-positive and Gram-negative bacteria. 35 One of the most potent GroEL/ES inhibitors that we discovered was compound 1 (Figure 3), which inhibited both the substrate refolding and ATPase functions of the chaperonin system. 33,35 Unfortunately, compound 1 was inactive against the panel of bacteria we tested against, suggesting it may not be a good candidate for antibacterial development.…”

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confidence: 99%

“…35 One of the most potent GroEL/ES inhibitors that we discovered was compound 1 (Figure 3), which inhibited both the substrate refolding and ATPase functions of the chaperonin system. 33,35 Unfortunately, compound 1 was inactive against the panel of bacteria we tested against, suggesting it may not be a good candidate for antibacterial development. 35 However, we found a related analog in the PubChem database where the benzimidazole core is replaced by a benzoxazole (Figure 3, compound 2e-p, PubChem CID #1098316).…”

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confidence: 99%

“…33,35 Unfortunately, compound 1 was inactive against the panel of bacteria we tested against, suggesting it may not be a good candidate for antibacterial development. 35 However, we found a related analog in the PubChem database where the benzimidazole core is replaced by a benzoxazole (Figure 3, compound 2e-p, PubChem CID #1098316). 34 While compound 2e-p has been evaluated in 285 assays, it was reported to be active in only 8 bioassays, suggesting this scaffold may be inherently selective and thus a promising candidate to explore for further drug development.…”

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confidence: 99%

“…41 From our previous antibacterial testing, we found that compound 1 exhibited moderate cytotoxicity to human liver (THLE-3) and kidney (HEK 293) cell lines in an established cell culture assay that measures compound cytotoxicity over a 72 h time course. 35 Therefore, in the present study, we developed a set of analogs to try to enhance their anti-parasitic effects against T. brucei while reducing off-target cytotoxicity to human liver and kidney cells. We synthesized two series of compound 1 analogs through simple coupling of sulfonyl chlorides with the 5-amino-2-(4aminophenyl)benzoxazole core (Scheme 1).…”

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confidence: 99%

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Targeting the HSP60/10 chaperonin systems of Trypanosoma brucei as a strategy for treating African sleeping sickness

Abdeen¹,

Salim²,

Mammadova³

et al. 2016

Bioorganic & Medicinal Chemistry Letters

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Trypanosoma brucei are protozoan parasites that cause African sleeping sickness in humans (also known as Human African Trypanosomiasis-HAT). Without treatment, T. brucei infections are fatal. There is an urgent need for new therapeutic strategies as current drugs are toxic, have complex treatment regimens, and are becoming less effective owing to rising antibiotic resistance in parasites. We hypothesize that targeting the HSP60/10 chaperonin systems in T. brucei is a viable anti-trypanosomal strategy as parasites rely on these stress response elements for their development and survival. We recently discovered several hundred inhibitors of the prototypical HSP60/10 chaperonin system from Escherichia coli, termed GroEL/ES. One of the most potent GroEL/ES inhibitors we discovered was compound 1. While examining the PubChem database, we found that a related analog, 2e-p, exhibited cytotoxicity to Leishmania major promastigotes, which are trypanosomatids highly related to Trypanosoma brucei. Through initial counter-screening, we found that compounds 1 and 2e-p were also cytotoxic to Trypanosoma brucei parasites (EC=7.9 and 3.1μM, respectively). These encouraging initial results prompted us to develop a library of inhibitor analogs and examine their anti-parasitic potential in vitro. Of the 49 new chaperonin inhibitors developed, 39% exhibit greater cytotoxicity to T. brucei parasites than parent compound 1. While many analogs exhibit moderate cytotoxicity to human liver and kidney cells, we identified molecular substructures to pursue for further medicinal chemistry optimization to increase the therapeutic windows of this novel class of chaperonin-targeting anti-parasitic candidates. An intriguing finding from this study is that suramin, the first-line drug for treating early stage T. brucei infections, is also a potent inhibitor of GroEL/ES and HSP60/10 chaperonin systems.

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Novel Antibacterial Targets in Protein Biogenesis Pathways

et al. 2021

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Antibiotic resistance has emerged as a global threat due to the ability of bacteria to quickly evolve in response to the selection pressure induced by anti‐infective drugs. Thus, there is an urgent need to develop new antibiotics against resistant bacteria. In this review, we discuss pathways involving bacterial protein biogenesis as attractive antibacterial targets since many of them are essential for bacterial survival and virulence. We discuss the structural understanding of various components associated with bacterial protein biogenesis, which in turn can be utilized for rational antibiotic design. We highlight efforts made towards developing inhibitors of these pathways with insights into future possibilities and challenges. We also briefly discuss other potential targets related to protein biogenesis.

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GroEL/ES inhibitors as potential antibiotics

Cited by 35 publications

References 50 publications

Serological Testing for Mycobacterial Heat Shock Protein Hsp65 Antibody in Health and Diseases

Serological Testing for Mycobacterial Heat Shock Protein Hsp65 Antibody in Health and Diseases

Targeting the HSP60/10 chaperonin systems of Trypanosoma brucei as a strategy for treating African sleeping sickness

Novel Antibacterial Targets in Protein Biogenesis Pathways

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