In Vitro Evolutionary Dynamics of C. albicans during Adaptation to Fluocnazole

Huang, Mian

2012 August 1900

Many drug-resistant mechanisms in Candida albicans (C. albicans), a clinical important fungal pathogen, have been well characterized. However, few studies investigated the emergence of drug resistance from the evolutionary perspective and little is known about the evolutionary trajectories during the adaptation to the drug. Here, we examined the evolutionary dynamics of C. albicans both in the presence and absence of fluconazole, a first line drug, using the visualizing evolution in real-time (VERT) method. Evolutionary dynamics of replicate C. albicans populations, either in the presence or absence of fluconazole, were determined and adaptive mutants arose in the populations were systematically isolated using the VERT method. Drug susceptibility assays were performed to measure the fluconazole minimum inhibitory concentration (MIC) for the adaptive isolates from drug-exposed populations. Analysis of the evolutionary dynamics revealed that mutations arose more frequently in the presence of the drug compared to the absence of the drug and the drug-resistant mutations occurred in independent lineages, suggesting a heterogeneous nature of the populations during the adaptation. In addition, fitness effects were evaluated for each adaptive mutant both in the presence and absence of drug and we found most of them gained significant increase in the drug resistance without a fitness cost in the absence of the drug. Interestingly, the aneuploidy and gross chromosomal rearrangements, common drug-resistant mechanisms, were not responsible for the increased resistance to fluconazole of most adaptive isolates, suggesting single-nucleotide polymorphisms (SNPs) or other stable unknown chromosomal rearrangements may contribute to the increased drug resistance.

Candida albicans

evolutionary dynamics

drug resistance

Antibiotic resistance in staphylococci associated with cats and dogs /

Malik, Seidu.

Unknown Date

Staphylococci are important opportunistic pathogens often found in the microflora of skin and mucosal surfaces of the upper respiratory tract of man and animals. The coagulase-postive species such as Staphylococcus aureus are capable of causing invasive (eg furuncles and bacteramia) and non-invasive (food poisoning and toxic shock syndrome) conditions in humans. In animals, S. intermedius and S. aureus have been implicated in a variety of conditions including pyoderma in dogs, mastitis in cows and skin infections in horses with S. intermedius being responsible for more than 95% of staphylococcal infections in dogs. / Thesis (PhD)--University of South Australia, 2006.

Staphylococcus.

Drug resistance in microorganisms.

Antibiotics in veterinary medicine.

Antibiotic resistance in enteric bacteria associated with pigs /

Hart, Wendy S.

Unknown Date

Thesis (MAppSc)--University of South Australia, 2001.

Drug resistance in microorganisms

Antibiotic residues

Swine

Induction of Drug Resistance and Differentiation in Human Leukaemia Cell Lines

January 1994

The ability of low, clinically relevant levels of the chemotherapeutic drugs epirubicin and vinblastine to induce drug resistance was examined in the K562. U937, KG-la and HEL human leukaemia cell lines. Treatment with epirubicin and vinblastine induced the MDR phenotype and P-glycoprotein expression in K562 and U937 cells. However this treatment had no effect on drug resistance in the P-glycoprotein expressing KG-la and HEL cells. In the U937 cells, drug resistant cells were not only MDR but were also resistant to other drugs including cisplatinum and chlorambucil which are not normally associated with MDR. The drug resistant U937 sublines were also sensitised to doxorubicin, cisplatinum and chlorambucil by buthionine sulphoximine (BSO), suggesting that glutathione-related mechanisms also contributed to resistance in these sublines. The U937 sublines also had an increased DNA content and an increased ability to recover from DNA damage, as determined by cell cycle analysis, indicating that the broad cross-resistance exhibited by these cells was due to the co-existence of multiple resistance mechanisms. Drug treatment induced changes in expression of differentiation associated antigens in all four cell lines. Treatment with inducers of differentiation (TPA, sodium butyrate, granulocyte-macrophage colony-stimulating factor; GM-CSF). Treatment of K562 and K562/E15B cells with TPA induced megakaryocytic differentiation, with increases in drug resistance, and increased P-glycoprotein expression in the K562/E15B subline. TPA induced monocytic differentiation in the U937 cells but not the U937/EIS subline, with increased P-glycoprotein expression and function in the U937/E15 cells but not the U937 cells. Staurosporine, an inhibitor of PKC, inhibited differentiation in these cell lines, but did not inhibit increases in P-glycoprotein expression, suggesting drug resistance was not mediated by PKC. Sodium butyrate induced erythroid differentiation, and increased P-glycoprotein expression in the K562/E15B cells. However at a higher concentration (15 mM) this was not accompanied by increased drug resistance. Granulocyte monocyte colony stimulating factor (GM-CSF) did not induce differentiation in the K562 cells or K562/E15B subline, although the K562/E15B cells became more drug resistant after treatment with GM-CSF. Treatment with GM-CSF induced differentiation in the U937/E15 subline but did not change drug resistance in either the U937 cells or the U937/EI5 subline. Therefore the P-glycoprotein expressing K562/E15B and U937/E15 sublines were more responsive to inducers of differentiation than the parental cell lines. Induction of differentiation therefore induced increases in P-glycoprotein expression and drug resistance, suggesting that expression of P-glycoprotein or a multidrug resistance phenotype was associated with differentiation.

Drug resistance

cancer cells

leukemia

chemotherapy.

Territory-wide Antibiotic Stewardship Programme and its effectiveness in public hospitals in Hong Kong /

Lo, Chiu-sing.

January 2007

Thesis (M. P. H.)--University of Hong Kong, 2007.

Genetic profiling of drug resistance in Plasmodium falciparum /

Certain, Laura K.

January 2007

Thesis (Ph. D.)--University of Washington, 2007. / Vita. Includes bibliographical references (leaves 173-196).

Applications of proteomics : identification of genes associated with anti-cancer drug resistance, liver development and regeneration /

Chow, Hoi-yee.

January 2006

Thesis (Ph. D.)--University of Hong Kong, 2007. / Also available online.

Characterization of aminoglycoside phosphotransferase APH(3')-IIIa : an enterococcal enzyme conferring resistance to aminoglycoside antibiotics /

McKay, Geoffrey A.

January 1999

Thesis (Ph.D.) -- McMaster University, 1999. / Includes bibliographical references (leaves 216-244). Also available via World Wide Web.

Comparsion [sic] of antibiotic sensitivity profiles, molecular typing patterns, and attribution of Salmonella enterica serotype Newport in the U.S., 2003-2006

Patel, Nehal J.

January 2007

Thesis (M.P.H.)--Georgia State University, 2007. / Title from file title page. Karen Gieseker, committee chair; Michael Eriksen, Peter Gerner-Smidt, Kelley Hise, committee members. Electronic text (105 p. : ill. (some col.)) : digital, PDF file. Description based on contents viewed Nov. 28, 2007. Includes bibliographical references (p.101-105).

Macrolide-lincosamide-streptogramin B resistance among staphylococcus aureus carried by children with atopic dermatitis /

Kwok, Chi-fong, Joyce.

January 2007

Thesis (M. Med. Sc.)--University of Hong Kong, 2008.