Beta-cyclodextrin derivatives as antibacterial agents

BACKGROUND OF THE INVENTION

1. Field of the Invention

The invention relates to development of new antibiotics against pathogenic bacteria.

2. Summary of the Related Art

Numerous bacteria are known to cause diseases in humans. Among these bacteria are Enterococcus faecium, Eschericia coli, Pseudomonas aeruginosa, Bacillus atrophaeus, Staphylococcus aureus, Salmonella choleraesuis, Bacillus anthrasis, and many others. A disturbing recent trend has been the development of resistance to existing antibiotics in numerous pathogenic bacteria. There is, therefore, a need for new antibiotics for which resistance has not yet emerged. Preferably, such antibiotics should be members of a new class of antibiotics, thus making evolutionary resistance to these antibiotics more difficult.

BRIEF SUMMARY OF THE INVENTION

The invention provides a new class of antibiotics to which pathogenic bacteria have not been exposed, and thus should not have developed resistance. This new class of antibiotics are derivatives of β-cyclodextrin (β-CD), which is a cyclic molecule comprising seven D-glucose units.

In a first aspect, the invention provides a compound having the formula
embedded image

wherein R₂is H, OH, OAc, O-lower alkyl, OMe, or O(CH₂CH₂O)_n; R₃is H, OH, OAc, O-lower alkyl, OMe, OSO₃Na, or NH₂; and R₆is N which is mono, di or tri-substituted with alkyl, aralkyl, aryl, heterocyclic ring or heterocyclic alkyl, and any of which substituents can be further substituted with N, O or S which can be further substituted with H, alkyl, aralkyl or aryl, wherein for each of R₂, R₃and R₆any one or more of the carbon atoms may be optionally replaced by S, N or O, and wherein _nis from about 1 to about 15, preferably from about 1 to about 10.

In a second aspect the invention provides pharmaceutical compositions. These compositions comprise one or more members of the compounds disclosed in the invention and a pharmaceutically acceptable carrier.

In a third aspect, the invention provides methods for using a compound or compounds having the formula:
embedded image

wherein R₂is H, OH, OAc, OMe, O-lower alkyl, or O(CH₂CH₂O)_n; R₃is H, OH, OAc, OMe, O-lower alkyl, OSO₃Na, or NH₂; and R₆is H, NH₂, S(CH₂)_mNH₂, I, N₃, SH, lower alkyl, S-alkylguanidyl, O-alkylguanidyl, S-aminoalkyl, O-aminoalkyl, aminoalkyl, O-lower alkyl, aralkyl, aryl, heterocyclic ring(s), OSO₃Na or N which is mono, di or tri-substituted with alkyl, aralkyl, aryl, heterocyclic ring or heterocyclic alkyl, and any of which substituents can be further substituted with N, O or S which can be further substituted with H, alkyl, aralkyl or aryl, wherein for each of R₂, R₃and R₆any one or more of the carbon atoms may be optionally replaced by S, N or O, and wherein _nis from about 1 to about 15, preferably from about 1 to about 10, and wherein _mis from about 1 to about 15, preferable from about 1 to about 10, as antimicrobial agents. In one embodiment of this aspect, the invention provides a method for inhibiting the growth of a bacterium. In a further embodiment of this aspect, the invention provides methods for treating a bacterial infection. In a further embodiment of this aspect, the invention provides methods for preventing a bacterial infection.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

The invention relates to development of new antibiotics against pathogenic bacteria. The invention provides a new class of antibiotics to which pathogenic bacteria have not been exposed, and thus should not have developed resistance. This new class of antibiotics are derivatives of β-cyclodextrin (β-CD), which is a cyclic molecule comprising seven D-glucose units.

As used herein, the term “physiologically acceptable” refers to a material that does not interfere with the effectiveness of the compounds of the first or third aspects of the invention and is compatible with a biological system such as a cell, cell culture, tissue, or organism. In certain embodiments, the biological system is a living organism, such as a mammal. In certain embodiments, the mammal is a human.

As used herein, the term “carrier” encompasses any excipient, diluent, filler, salt, buffer, stabilizer, solubilizer, lipid, or other material well known in the art for use in pharmaceutical formulations. It will be understood that the characteristics of the carrier, excipient, or diluent will depend on the route of administration for a particular application. The preparation of pharmaceutically acceptable formulations containing these materials is described in, e.g., Remington's Pharmaceutical Sciences, 18th Edition, ed. A. Gennaro, Mack Publishing Co., Easton, Pa., 1990, ISBN: 0-912734-04-3.

In a third aspect, the invention provides methods for using a compound or compounds of the first and second aspects of the invention as antimicrobial agents. In one embodiment of this aspect, the invention provides a method for inhibiting the growth of a bacterium. The method according to this embodiment of the invention comprises contacting the bacteria with one or more members of a compound having the formula
embedded image

wherein R₂is H, OH, OAc, OMe, O-lower alkyl, or O(CH₂CH₂O)_n; R₃is H, OH, OAc, OMe, O-lower alkyl, OSO₃Na, or NH₂; and R₆is H, NH₂, S(CH₂)_mNH₂, I, N₃, SH, lower alkyl, S-alkylguanidyl, O-alkylguanidyl, S-aminoalkyl, O-aminoalkyl, aminoalkyl, O-lower alkyl, aralkyl, aryl, heterocyclic ring(s), OSO₃Na or N which is mono, di or tri-substituted with alkyl, aralkyl, aryl, heterocyclic ring or heterocyclic alkyl, and any of which substituents can be further substituted with N, O or S which can be further substituted with H, alkyl, aralkyl or aryl, wherein for each of R₂, R₃and R₆any one or more of the carbon atoms may be optionally replaced by S, N or O, and wherein _nis from about 1 to about 15, preferably from about 1 to about 10, and wherein _mis from about 1 to about 15, preferable from about 1 to about 10.

For purposes of the invention, the term “lower alkyl” means an alkyl group from 1 to 7 carbon atoms. The terms “alkyl” and “aryl” include alkyl or aryl groups which may be substituted or unsubstituted. Preferred substitutions include, without limitation, substitution with nitrogen containing moieties, including amino groups, which may be mono or disubstituted, preferably with alkyl or aryl groups. Also, for purposes of the invention the term “alkyl” includes chains of 1-7 atoms with one or more nitrogen atoms and the remainder carbon atoms.

In a further embodiment of this aspect, the invention provides methods for treating a bacterial infection. The method according to this embodiment of the invention comprises administering to a mammal with a bacterial infection one or more members of a compound having the formula
embedded image

wherein R₂is H, OH, OAc, OMe, O-lower alkyl, or O(CH₂CH₂O)_n; R₃is H, OH, OAc, OMe, O-lower alkyl, OSO₃Na, or NH₂; and R₆is H, NH₂, S(CH₂)_mNH₂, I, N₃, SH, lower alkyl, S-alkylguanidyl, O-alkylguanidyl, S-aminoalkyl, O-aminoalkyl, aminoalkyl, O-lower alkyl, aralkyl, aryl, heterocyclic ring(s), OSO₃Na or N which is mono, di or tri-substituted with alkyl, aralkyl, aryl, heterocyclic ring or heterocyclic alkyl, and any of which substituents can be further substituted with N, O or S which can be further substituted with H, alkyl, aralkyl or aryl, wherein for each of R₂, R₃and R₆any one or more of the carbon atoms may be optionally replaced by S, N or O, and wherein _nis from about 1 to about 15, preferably from about 1 to about 10, and wherein _mis from about 1 to about 15, preferable from about 1 to about 10.

In a further embodiment of this aspect, the invention provides methods for preventing a bacterial infection. The method according to this embodiment of the invention comprises administering to a mammal susceptible to a bacterial infection one or more members of a compound having the formula
embedded image

wherein R₂is H, OH, OAc, OMe, O-lower alkyl, or O(CH₂CH₂O)_n; R₃is H, OH, OAc, OMe, O-lower alkyl, OSO₃Na, or NH₂; and R₆is H, NH₂, S(CH₂)_mNH₂, I, N₃, SH, lower alkyl, S-alkylguanidyl, O-alkylguanidyl, S-aminoalkyl, O-aminoalkyl, aminoalkyl, O-lower alkyl, aralkyl, aryl, heterocyclic ring(s), OSO₃Na or N which is mono, di or tri-substituted with alkyl, aralkyl, aryl, heterocyclic ring or heterocyclic alkyl, and any of which substituents can be further substituted with N, O or S which can be further substituted with H, alkyl, aralkyl or aryl, wherein for each of R₂, R₃and R₆any one or more of the carbon atoms may be optionally replaced by S, N or O, and wherein _nis from about 1 to about 15, preferably from about 1 to about 10, and wherein _mis from about 1 to about 15, preferable from about 1 to about 10.

In the methods according to this aspect of the invention the bacteria is in a mammal. Preferably, the mammal is a human.

In the methods according to this aspect of the invention, administration of the compound can be by any suitable route, including, without limitation, parenteral, oral, sublingual, transdermal, topical, intranasal, aerosol, intraocular, intratracheal, intrarectal or vaginal. Administration of the therapeutic compositions can be carried out using known procedures at dosages and for periods of time effective to reduce symptoms or surrogate markers of the infection. A doctor can determine the appropriate dose to administer or therapeutic protocol useful for preventing or preventing a bacterial infection. It may be desirable to administer simultaneously, or sequentially a therapeutically effective amount of one or more of the therapeutic compositions of the invention to an individual as a single treatment episode.

In a fourth aspect, the invention provides methods for potentiating the activity of antibiotics to inhibit the growth of a bacterium which are resistant to clinically used antibiotics, to treat or prevent an infection by these bacteria. The methods according to this aspect of the invention comprise contacting the bacterium with said antibiotic and one or more members of a compound having the formula
embedded image

wherein R₂is H, OH, OAc, OMe, O-lower alkyl, or O(CH₂CH₂O)_n; R₃is H, OH, OAc, OMe, O-lower alkyl, OSO₃Na, or NH₂; and R₆is H, NH₂, S(CH₂)_mNH₂, I, N₃, SH, lower alkyl, S-alkylguanidyl, O-alkylguanidyl, S-aminoalkyl, O-aminoalkyl, aminoalkyl, O-lower alkyl, aralkyl, aryl, heterocyclic ring(s), OSO₃Na or N which is mono, di or tri-substituted with alkyl, aralkyl, aryl, heterocyclic ring or heterocyclic alkyl, and any of which substituents can be further substituted with N, O or S which can be further substituted with H, alkyl, aralkyl or aryl, wherein for each of R₂, R₃and R₆any one or more of the carbon atoms may be optionally replaced by S, N or O, and wherein _nis from about 1 to about 15, preferably from about 1 to about 10, and wherein _mis from about 1 to about 15, preferable from about 1 to about 10.

For purposes of the invention, the term “resistant” or “resistance” to a bacterium or bacterial infection to an antibiotic includes a complete resistance to the antibiotic or a partial resistance which is defined herein as a circumstance in which the MIC of an antibiotic toward the organism in question has increased.

For purposes herein, potentiation may be defined as a circumstance in which a compound substantially lowers the MIC of an antibacterial agent toward one or more organisms. It includes the case in which it effectively restores the therapeutic utility of an antibacterial agent whose utility has been compromised by bacterial resistance.

In any of the methods according to the invention, one or more members of compounds of the invention can be administered in combination with any other antibiotic useful for treating the disease or condition that does not diminish the antimicrobial effect of the compound. For purposes of this aspect of the invention, the term “in combination with” means in the course of treating the same disease in the same patient, and includes administering the compound and an antibiotic in any order, including simultaneous administration, as well as any temporally spaced order, for example, from sequentially with one immediately following the other to up to several days apart. Such combination treatment may also include more than a single administration of the compound, and independently the antibiotic. The administration of the compound and antibiotic may be by the same or different routes.

In the methods according to this aspect of the invention the bacteria is in a mammal. Preferably, the mammal is a human.

In certain aspects of the methods according to the invention, it is desirable to have antibiotics with a relatively broad spectrum, so that a variety of different bacterial infection can be treated. In other aspects, such as protection against bioterrorism, it may be desirable to have antibiotics with a narrow spectrum, specific for likely bioterrorism organisms, so that protection from the bacteria may be obtained while preserving the normal flora in the body. The invention provides methods for achieving each of these goals.

The following examples are intended to further illustrate certain particularly preferred embodiments of the invention and are not intended to limit the scope of the invention.

EXAMPLE 1
Bacterial Growth Standardization

One to three colonies of bacteria were picked from an Mueller-Hinton or Brain Heart infusion agar plate (depending on the bacterial strain) and transferred to 3 ml Mueller-Hinton broth or Brain Heart infusion media (depending on the bacterial strain). Bacteria were allowed to grow for 2-4 hours in an incubator at 37° C. Bacteria-inoculated media were dispersed in 0.9% saline to match McFarland standard density. 100 μl standardized inoculation was added to 20 ml media (dilution 1). 10 μl of the new dilution was added to 990 μl media and mixed (dilution 2). 10 μl of dilution 2 was spread on an agar plate and allowed to grow overnight. Colonies were then plated.

EXAMPLE 2
Bacterial Panel Testing

Test compound was diluted to 10 μg/ml in dimethylsulfoxide. Four μl of diluted test compound was loaded into column 2 of a 96 well NUNC microplate, as shown in Table 1 below. Four μl of Rifampicin antibiotic was loaded into row H, column 2.

TABLE 196 well NUNC microplate set-up, Concentration in μg/ml123456789101112A0200100502512.56.253.121.560.780.390.20B0200100502512.56.253.121.560.780.390.20C0200100502512.56.253.121.560.780.390.20D0200100502512.56.253.121.560.780.390.20E0200100502512.56.253.121.560.780.390.20F0200100502512.56.253.121.560.780.390.20G0200100502512.56.253.121.560.780.390.20H0200100502512.56.253.121.560.780.390.20rifampicin

All wells were then filled with 100 μl of inoculated media (dilution 1 from Example 1). A further 100 μl of the inoculated media was then added to column 2 and the contents are pipetted to thoroughly mix the contents. A full 100 μl was then transferred from column 2 and mixed into column 3. This process was continued from left to right until columns 2-12 were serially diluted, and the final draw from column 12 was discarded. The plates were covered with 3M sealing tape (plates containing Enterococcus faecium were sealed with Air Pore sealing tape) and allowed to grow for 20-24 hours. Cytotoxic wells (clear wells) are then scored and the potency of the compound was determined. The results are shown in Table 2 below. These results show that while some compounds were inactive, others demonstrated either broad spectrum or narrow spectrum activity.

TABLE 2Activity of test compounds (MICs in μg/mL)MammalianCytotoxicity*CompoundPASASCECBAEFIC50 (μg/mL) embedded image

>200>200>200>200>200>200PP5000 embedded image

6.25-3.12>200>200200-100100-50 >200720PP5001 embedded image

>200>200>200>20012.5-6.25>200829PP5002 embedded image

>200>200>200100-50 3.12-1.56>200191PP5003 embedded image

>200>200>200>2001.56-0.78>200198PP5004 embedded image

>200>200>200>200200-100>200690PP5005 embedded image

>200>200>200>20050-25>200215PP5006 embedded image

>200>200>200>200 25-12.5>200>2000PP5007 embedded image

>200>200>200>200 25-12.5>200510PP5008 embedded image

>200>200>200>200200-100>200755PP5009 embedded image

>200100-50 >200>200200-100>200780PP5010 embedded image

>2003.12-1.5650-25 25-12.51.56-0.7850-25840PP5011 embedded image

>200>200>200>200>200>200193PP5012 embedded image

>200>200>200>200>200>200144PP5013 embedded image

>200>200>200>200<0.2>200PP5014 embedded image

>20050-25>200>200100-50 >2002116PP5015 embedded image

>200>200>200>200200-100>200PP5016 embedded image

>200>200>200>200>200>200PP5017 embedded image

>200>200>200>200100-50 >200PP5018 embedded image

>200>200>200>200 25-12.5>200524PP5019 embedded image

>200>200>200>200200-100>200PP5020 embedded image

>200>200>200>200>200>200PP5021 embedded image

>200>200>200>20050-25>200PP5026 embedded image

>200>200 25-12.550-251.56-0.78>200321PP5027 embedded image

>200>200>200>200 25-12.5>2002990PP5028 embedded image

>200>200>200>200>200>200PP5029 embedded image

>200>200>200>200>200>200PP5030 embedded image

>200>200>200>20012.5-6.25>200PP5031 embedded image

>200>200>200>200>200>200PP5032 embedded image

>200>200>200>200>200>200PP5033 embedded image

>200>200>200>200 25-12.5>200480PP5035 embedded image

>200>200>200>200>200>200PP5036 embedded image

>200>200>200>200>200>200PP5037 embedded image

>200>200>200>200200-100>200PP5038 embedded image

>200>200>200>200>200>200PP5039 embedded image

>200>200100-50 50-25 25-12.5>200PP5040 embedded image

100-50 >200>200>20050-25>200860PP5041 embedded image

>200>200>200>200>200>200PP5042 embedded image

>200>200>200>200>200>200PP5043 embedded image

>200>200>200>200>200>200PP5044 embedded image

>200200-100100-50 200-10012.5-6.25—PP5046 embedded image

>200>200>200>20050-25—PP5047 embedded image

>20050-25100-50 >2006.25-3.12—PP5048 embedded image

>200>200>200>200100-50 PP5049 embedded image

>200>200>200>200>200>200PP5050 embedded image

>200>200>200>20012.5-6.25>200PP5051 embedded image

>200>200>200>200 25-12.5>200PP5052 embedded image

>200>200>200>200>200>200PP5053 embedded image

>200>200>200>200>200>200PP5054 embedded image

>200>200>200>200>200>200PP5055 embedded image

>200>200>200>200>200>200PP5056 embedded image

200-100>200>200>200>200>200PP5057 embedded image

>200>200>200>200200-100>200PP5058 embedded image

>200>200>200>200100-50 >200PP5059 embedded image

>200>200>200>200>200>200PP5060 embedded image

>200>200>200>200>200>200PP5061 embedded image

>200>200>200>200200-100>200PP5062 embedded image

>200>200>200>200>200>200PP5063 embedded image

>200200-100100-50 200-100100-50 >200PP5064 embedded image

>200>200>200>200>200>200PP5065 embedded image

>200>200>200>200>200>200PP5066 embedded image

>200>200>200>200>200>200PP5067 embedded image

>200>200>200>200>200>200PP5068 embedded image

>200>200>200>200>200>200PP5069 embedded image

>2003.12-1.56 25-12.512.5-6.251.56-0.786.25-3.1243PP5070 embedded image

>200>200>200>200>200>200PP5071 embedded image

>2006.25-3.12200-100100-50 1.56-0.786.25-3.12127PP5072 embedded image

>2003.12-1.5650-2550-251.56-0.786.35-3.12129PP5073 embedded image

>2006.25-3.1250-25100-50 6.25-3.126.25-3.12123PP5074 embedded image

>200100-50 >200>20050-25200-100PP5075 embedded image

>20012.5-6.25>200>2006.25-3.1212.5-6.25398PP5076 embedded image

>200>200>200>200>200>200PP5077 embedded image

>200>200>200>200100-50 >200PP5078 embedded image

>200 25-12.5>200>20012.5-6.25 25-12.5317PP5079 embedded image

>200>200>200>20012.5-6.2550-25PP5080 embedded image

>200200-100>200>20050-25>200PP5084 embedded image

>20012.5-6.25200-100>2006.25-3.12>200PP5085 embedded image

>20050-25>200>20050-25100-50 PP5086 embedded image

>200>200>200>200>200>200PP5087 embedded image

>200200-100>200>200>200>200PP5088 embedded image

>200200-100>200>200>200>200PP5089 embedded image

>2006.25-3.12>200>2003.12-1.5612.5-6.25PP5093 embedded image

>2003.12-1.56100-50 100-50 3.12-1.561.56-0.78PP5094 embedded image

>200>200>200>200>200>200PP5096 embedded image

>20012.5-6.25>200>2006.25-3.12100-50 PP5097 embedded image

>2003.12-1.56>200100-50 1.56-0.78 25-12.5378PP5098 embedded image

>200 25-12.5>200>20012.5-6.2550-25PP5099 embedded image

100-50 50-25100-50 100-50 50-25>200PP5100 embedded image

>200>200>200>200>200>200PP5101 embedded image

>200200-100>200>200100-50 >200PP5102 embedded image

>20012.5-6.25>200>20012.5-6.2550-25PP5103 embedded image

>200 25-12.5>200>200 25-12.5>200PP5104 embedded image

>2003.12-1.56>20050-251.56-0.7812.5-6.25376PP5105 embedded image

>200>200>200>200200-100>200PP5106 embedded image

>20012.5-6.25 25-12.5 25-12.56.25-3.12 25-12.5105PP5107 embedded image

>20012.5-6.25>200100-50 6.25-3.12 25-12.5PP5108 embedded image

>20012.5-6.25>200>20012.5-6.25 25-12.5PP5109 embedded image

>20012.5-6.25>200>2006.25-3.12 25-12.5PP5110 embedded image

>200>200>200>200>200>200PP5111 embedded image

>200>200>200>20012.5-6.25>200PP5112 embedded image

100-50 >200>200>200>200>200109.3PP5113 embedded image

100-50 >200200-10050-256.25-3.12>20056.2PP5114 embedded image

200-100200-100>20050-256.25-3.12>20054.3PP5115 embedded image

>200>200>200>200>200>200PP5116 embedded image

>2006.25-3.12>200200-1003.12-1.56100-50 373PP5117 embedded image

>2006.25-3.12200-100100-50 3.12-1.56100-50 282PP5118 embedded image

>200>200>200>200200-100>200PP5119 embedded image

>200>200>200>200>200>200PP5120 embedded image

>200>200>200>20050-25>200589PP5121 embedded image

>2006.25-3.12 25-12.5 25-12.53.12-1.5650-25297PP5122 embedded image

>2006.25-3.12>200200-1003.12-1.56200-100297PP5123 embedded image

200-100>200>200>20050-25>200PP5124 embedded image

>2003.12-1.56100-50 50-253.12-1.5612.5-6.25PP5125 embedded image

>20012.5-6.25100-50 200-100 25-12.512.5-6.25PP5126 embedded image

>2006.25-3.12100-50 200-10012.5-6.256.25-3.12PP5127 embedded image

>200>200>200100-50 50-25>200PP5128 embedded image

>200200-100>200>20012.5-6.25>200PP5129 embedded image

>2006.25-3.12>200100-50 6.25-3.126.25-3.12PP5130 embedded image

>20012.5-6.25>200>20012.5-6.2512.5-6.25PP5131 embedded image

>200100-50 >200>20050-25>200PP5132 embedded image

6.25-3.12 25-12.53.12-1.563.12-1.561.56-0.78100-50 PP5133 embedded image

25-12.512.5-6.256.25-3.126.25-3.126.25-3.1212.5-6.25PP5134 embedded image

100-50 25-12.5 25-12.5 25-12.512.5-6.2550-2532.4PP5135 embedded image

>20012.5-6.25200-100200-1003.12-1.56>200PP5136 embedded image

12.5-6.2512.5-6.25200-100>20012.5-6.2512.5-6.25PP5137 embedded image

>100>100>100>100100-50 >100PP5138 embedded image

>200>200>200>200>200>200PP5139 embedded image

>100 25-12.550-2550-253.12-1.56>100193.5PP5140 embedded image

>200>200>200100-50 12.5-6.25>200PP5145
*Lung cancer cells A549

EXAMPLE 3
Potentiation of Clinically Used Antibiotics by Compounds vs. Clinical Isolates of Pseudomonas aeruginosa

Numerous pathogenic bacteria have developed a resistance to many clinically used antibiotics. Following the protocols described herein, various compounds were mixed with clinically used antibiotics to treat Pseudomonas aeruginosa (P. aeruginosa). The results are shown in Tables 3 and 4 below. These results demonstrate that compounds of the invention are able to potentiate the activity of known antibiotics.

TABLE 3Activity of known antibiotics alone or in combination with compoundsof the inventionP. aeruginosaTest Compounds(susceptible clinical isolate)Methicillin>100Methicillin + PP5027 25-12.5Methicillin + PP5114 25-12.5Methicillin + PP51356.25-3.12Methicillin + PP5140100-50 Penicillin V>100Penicillin V + PP502750-25Penicillin V + PP511450-25Penicillin V + PP5135 25-12.5Penicillin V + PP514050-25Vancomycin>100Vancomycin + PP502712.5-6.25Vancomycin + PP5114 25-12.5Vancomycin + PP51353.12-1.56Vancomycin + PP5140100-50

TABLE 4

Activity of known antibiotics alone or in combination with compounds

of the invention (AG = Aminoglycoside)

Multi-drug

MIC μg/mL
Susceptible
AG Resistant
Resistant

Chloramphenicol
50-25
50-25
100-50

Chloramphenicol + PP5027
01.56-0.78
0.2-0.1
100-50

Chloramphenicol + PP5113
3.12-1.56
12.5-6.25
12.5-6.25

Chloramphenicol + PP5114
6.25-3.12
6.25-3.12
12.5-6.25

Chloramphenicol + PP5115
50-25
3.12-1.56
12.5-6.25

Chloramphenicol + PP5121
50-25
50-25
100-50

Norfloxacin
6.25-3.12
1.56-0.78
>100

Norfloxacin + PP5027
3.12-1.56
<0.1
>100

Norfloxacin + PP5113
0.78-0.39
0.78-0.39
>100

Norfloxacin + PP5114
0.78-0.39
0.2-0.1
>100

Norfloxacin + PP5115
6.25-3.12
3.12-1.56
>100

Norfloxacin + PP5121
6.25-3.12
1.56-0.78
>100

Tobramycin
0.39-0.2
12.5-6.25
>100

Tobramycin + PP5027
0.78-0.39
0.2-0.1
>100

Tobramycin + PP5113
<0.1
25-12.5
100-50

Tobramycin + PP5114
<0.1
3.12-1.56
>100

Tobramycin + PP5115
<0.1
3.12-1.56
>100

Tobramycin + PP5121
0.39-0.2
12.5-6.25
>100

EXAMPLE 4
Compounds Retain Activity Against Methicillin Resistant

Methicillin-resistant staphylococcus aureus is a bacterial infection resistant to antibiotic methicillin and can no longer be killed by this antiobiotic. Following the protocols described herein, various compounds were used antibiotics to treat Staphylococcus aureus (Methicillin resistant). The results are shown in Table 5 below. These results below demonstrate that compounds of the invention are able to retain activity against Methicillin resistance.

TABLE 5Activity of compounds against Methicillin ResistanceStaphylococcus aureus*Staphylococcus aureus(susceptible)(Methicillin resistant)CompoundMIC μg/mLCompoundMIC μg/mLPP50733.12-1.56PP50733.12-1.56PP50943.12-1.56PP50943.12-1.56PP50983.12-1.56PP50986.25-3.12PP51053.12-1.56PP51053.12-1.56PP51253.12-1.56PP51256.25-3.12
*ATCC 700698

Beta-cyclodextrin derivatives as antibacterial agents

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