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Drug Therapy of Experimental Tuberculosis (TB): Improved Outcome by Combining SQ109, a New Diamine Antibiotic, with Existing TB Drugs

Sequella, Inc., Rockville, Maryland 20850,¹ Central Research Institute for Tuberculosis, Moscow 107564, Russia²

Received 24 October 2006/ Returned for modification 27 November 2006/ Accepted 13 January 2007

	ABSTRACT

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Substitution of the new diamine antibiotic SQ109 for ethambutol in a mouse model of chronic tuberculosis (TB) improved efficacy of combination drug therapy with first-line TB drugs rifampin and isoniazid, with or without pyrazinamide: at 8 weeks, lung bacteria were 1.5 log₁₀ lower in SQ109-containing regimens.

	TEXT

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New antituberculosis drug regimens are clearly needed to reduce the therapy time interval required for a durable cure and to treat the expanding problem of drug- and multidrug-resistant (MDR) Mycobacterium tuberculosis strains. Several new drug candidates in development show comparable or better performance than currently available antitubercular agents both in vitro and in animal models of tuberculosis (TB) and are effective against MDR mycobacterial strains (1, 5, 11, 16, 17). For the past several years, we have been characterizing the properties of a new diamine drug candidate with antitubercular activity, SQ109 (4, 7, 8, 10, 14). This new drug with a cell wall mode of action has excellent in vitro activity against both drug-sensitive, single-drug-resistant, and MDR M. tuberculosis strains (more than 50, including laboratory strains and clinical isolates), with a MIC range of 0.16 to 0.64 µg/ml against all M. tuberculosis isolates tested. Moreover, SQ109 by itself at 10 mg/kg of body weight was able to reduce the number of lung CFU by over 1.5 to 2 log₁₀ in a chronic mouse model of TB, activity that was similar to monotherapy with ethambutol (EMB) at 100 mg/kg (7, 14).

Recently we reported marked in vitro synergistic activity of SQ109 with isoniazid (INH) and rifampin (RIF) and additive activity with streptomycin (4). In preliminary studies to evaluate any synergistic activity with front-line TB drugs in vivo, we used a screening mouse model that followed weight loss as an indicator of TB severity (2, 12). Similar to in vitro observations of synergy, combination therapy with SQ109-containing regimens was also better at preventing TB-induced weight loss than the standard drug regimens (13).

In this report, we compared the efficacy of TB therapy with three- and four-drug combinations where SQ109 replaced EMB in the more standard chronic mouse model of TB.

Groups of C57BL/6 female mice were inoculated intravenously with M. tuberculosis H37Rv and treated each day for 5 days/week with saline (untreated controls; six mice/time point), individual drugs (six mice/time point), or drug combinations (six mice/time point) beginning 3 weeks after infection and continuing for 4 or 8 weeks. To assess efficacy of treatment, we evaluated the average number of M. tuberculosis CFU in lungs of six mice/treatment each week during the course of therapy.

In the first set of experiments, we evaluated CFU in lungs of mice infected with 5 x 10⁴ CFU M. tuberculosis H37Rv and treated with INH alone or with a combination of INH plus RIF, INH plus RIF plus EMB, or INH plus RIF plus SQ109 over 4 weeks (Table 1). INH was used at 25 mg/kg; RIF was used at 20 mg/kg; EMB was used at its minimal effective dose in mice, 100 mg/kg; SQ109 was used at its minimum effective dose, 10 mg/kg. The combination of INH plus RIF plus SQ109 was better than and statistically different from INH plus RIF plus EMB at weeks 2, 3, and 4. At 4 weeks, the average number of viable M. tuberculosis in lungs of untreated mice was 6.42 log₁₀ CFU; lungs of mice treated with INH contained an average 4.61 log₁₀ CFU, the INH plus RIF group had an average 4.27 log₁₀ CFU, the INH plus RIF plus EMB group had 3.86 log₁₀ CFU, and the INH plus RIF plus SQ109 group had 3.26 log₁₀ CFU, 0.6 log₁₀ lower than the standard drug combination (Table 1). In terms of CFU counts, that half-log decrease in CFU translated into a fourfold decrease in the number of viable bacteria: 7,330 in mice treated with INH plus RIF plus EMB versus 1,830 in mice treated with INH plus RIF plus SQ109. Moreover, the combination of INH plus RIF plus SQ109 resulted in the same CFU level in lungs at week 3 as in the INH plus RIF plus EMB group at week 4, a full week earlier. Two other 4-week experiments with the identical three-drug regimen demonstrated similar results: differences between log₁₀ CFU of mice treated with INH plus RIF plus EMB and INH plus RIF plus SQ109 were 0.44 and 0.50 (experiments 2 and 3, respectively), with the SQ109-containing regimen showing better elimination of bacteria from the lung.

View larger version (9K): [in this window] [in a new window]   FIG. 1. Efficacy of four-drug combination treatment of mice infected with M. tuberculosis H37Rv. Differences between CFU recovered from lungs of mice treated with the EMB-containing regimen and the SQ109-containing regimen were significant (4-week treatment, P = 0.001; 6-week treatment, 1.5 log10 CFU difference, P = 0.022; 8-week treatment, 1.5 log10 CFU difference, P < 0.001). Ó, INH (25 mg/kg) plus RIF (20 mg/kg).

The combination of SQ109 with INH, RIF, and PZA in this study provided a new and very effective anti-TB intensive phase treatment regimen that achieved a better and faster rate of mycobacterial kill than the therapeutic regimen of INH plus RIF plus EMB plus PZA. The long half-life of SQ109 in vivo (26 h in beagle dogs [6]) suggests that replacing RIF with longer-acting rifamycins that can be administered weekly in SQ109 combination therapies might also improve the timing of drug delivery for a TB therapy that includes SQ109 (9, 15). The half-life of SQ109 in humans is not yet known, but ongoing phase 1 safety studies of SQ109 in human volunteers will provide these data in the next several months.

	ACKNOWLEDGMENTS

 
This work was generously supported by the National Institutes of Health, NIAID challenge grant UC1 AI-049514-01 ("Second generation antibiotics from ethambutol"), SBIR phase I grant R43 AI060250-01 ("Development of dipiperidines as a new class of anti-TB drugs"), and corporate matching funds.

	FOOTNOTES

 
* Corresponding author. Mailing address: Sequella, Inc., 9610 Medical Center Drive, Suite 200, Rockville, MD 20850. Phone: (301) 762-7776. Fax: (301) 762-7778. E-mail: borisnikonenko{at}sequella.com

Published ahead of print on 22 January 2007.

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This Article Abstract Full Text (PDF) Other Versions of this Article: AAC.01326-06v1 51/4/1563    most recent Alert me when this article is cited Alert me if a correction is posted Services Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Copyright Information Books from ASM Press MicrobeWorld Citing Articles Citing Articles via Google Scholar Google Scholar Articles by Nikonenko, B. V. Articles by Nacy, C. A. Search for Related Content PubMed PubMed Citation Articles by Nikonenko, B. V. Articles by Nacy, C. A.