Synergistic Activity between Statins and Bisphosphonates against Acute Experimental Toxoplasmosis

Li, Zhu-Hong; Li, Catherine; Szajnman, Sergio H.; Rodríguez, Juan B.; Moreno, Silvia N.J.

doi:10.1128/aac.02628-16

Cited by 25 publications

(37 citation statements)

References 35 publications

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“…Moreover, a strong synergistic effect was observed when another sulfur‐containing compound was assayed against T. gondii . In this context, 1‐[( n ‐heptylthio)ethyl]‐1,1‐biphosphonate ( 77 , C7S), when used in combination with atorvastatin (a potent inhibitor of the host 3‐hydroxy‐3‐methylglutaryl‐coenzyme A reductase), was found to have high activity against the hypervirulent RH strain of T. gondii in in vivo assays (Figure ) . This synergistic effect had been observed previously with zoledronic acid ( 61 , see Figure ) …”

Section: Bisphosphonatessupporting

confidence: 64%

The Role of the Phosphorus Atom in Drug Design

2019

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Although the phosphorus atom is found in a variety of oxidation states, most of the phosphorus‐containing molecules of pharmacological importance possess phosphorus in the form of phosphonate or phosphinate functional groups, or in a major oxidation state as a phosphate group. The most common occurrence of phosphorus in drugs is either in prodrugs or in compounds for which the phosphorus atom plays a role in the biological activity, such as in modified nucleotides, in metabolically stable analogues of metabolites bearing phosphate groups, and as bioisosteric analogues of carboxyl groups.

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Section: Bisphosphonatessupporting

confidence: 64%

The Role of the Phosphorus Atom in Drug Design

2019

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“…A similar observation was made in T. gondii (an apicomplexan), as the intracellular tachyzoites were capable of salvaging isoprenoids to support growth in fibroblasts but not macrophages [26]. Such discoveries have promoted the development of drug combinations that act synergistically by inhibiting both host and parasite isoprenoid synthesis [53].…”

Section: Discussionmentioning

confidence: 62%

Farnesyl pyrophosphate synthase is essential for the promastigote and amastigote stages in Leishmania major

Mukherjee

Basu

Zhang

2019

Molecular and Biochemical Parasitology

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Isoprenoid synthesis provides a diverse class of biomolecules including sterols, dolichols, ubiquinones and prenyl groups. The enzyme farnesyl pyrophosphate synthase (FPPS) catalyzes the formation of farnesyl pyrophosphate, a key intermediate for the biosynthesis of all isoprenoids. In Leishmania, FPPS is considered the main target of nitrogen containing bisphosphonates, yet the essentiality of this enzyme remains untested. Using a facilitated knockout approach, we carried out the genetic analysis of FPPS in Leishmania major. Our data indicated that chromosomal null mutants for FPPS could only be generated in presence of an episomally expressed FPPS. Longterm retention of the episome by the chromosomal FPPS-null mutants in culture and in infected BALB/c mice suggests that FPPS is indispensable. In addition, applying negative selection pressure failed to induce the loss of ectopic FPPS in the chromosomal FPPS-null mutants, although it led to significant growth delay in culture and in mice. Together, our findings have confirmed the essentiality of FPPS in both promastigotes and amastigotes in L. major and thus validate its potential as a drug target for the treatment of cutaneous leishmaniasis.

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“…parkeri, the parasite Cryptosporidium parvum lacks the canonical protozoan isoprenoid pathway and has been shown to be sensitive to statins (52). Interestingly, the facultative intracellular protozoan parasite Toxoplasma gondii, which encodes the MEP isoprenoid pathway within a membrane-bound organelle called the apicoplast, has been shown to be sensitive to statins when the parasite is intracellular (53, 54), suggesting that host metabolite scavenging is still advantageous for pathogens with intact pathways. In the future, bioinformatic analyses may identify other intracellular bacteria that have incomplete upstream isoprenoid pathways and intact downstream isoprenoid pathways and thus may also be sensitive to statins.…”

Section: Discussionmentioning

confidence: 99%

A Metabolic Dependency for Host Isoprenoids in the Obligate Intracellular Pathogen Rickettsia parkeri Underlies a Sensitivity to the Statin Class of Host-Targeted Therapeutics

Ahyong

Berdan

Burke

et al. 2019

mSphere

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Obligate intracellular pathogens, which include viruses as well as certain bacteria and eukaryotes, are a subset of infectious microbes that are metabolically dependent on and unable to grow outside an infected host cell because they have lost or lack essential biosynthetic pathways. In this study, we describe a metabolic dependency of the bacterial pathogen Rickettsia parkeri on host isoprenoid molecules that are used in the biosynthesis of downstream products, including cholesterol, steroid hormones, and heme. Bacteria make products from isoprenoids, such as an essential lipid carrier for making the bacterial cell wall. We show that bacterial metabolic dependency can represent a potential Achilles’ heel and that inhibiting host isoprenoid biosynthesis with the FDA-approved statin class of drugs inhibits bacterial growth by interfering with the integrity of the cell wall. This work supports the potential to treat infections by obligate intracellular pathogens through inhibition of host biosynthetic pathways that are susceptible to parasitism.

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Synergistic Activity between Statins and Bisphosphonates against Acute Experimental Toxoplasmosis

Cited by 25 publications

References 35 publications

The Role of the Phosphorus Atom in Drug Design

The Role of the Phosphorus Atom in Drug Design

Farnesyl pyrophosphate synthase is essential for the promastigote and amastigote stages in Leishmania major

A Metabolic Dependency for Host Isoprenoids in the Obligate Intracellular Pathogen Rickettsia parkeri Underlies a Sensitivity to the Statin Class of Host-Targeted Therapeutics

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