Abstract

~&crobial mats are conspicuous benthic communities composed almost entirely of prokaryotic microorganisms. These mats develop in extreme environments which limit the growth of Eukaryotic organisms. Nficrobial mats are found in high temperature, high salinity, high alkalinity, and high sulfide environments where microorganisms can accrete due to the absence of predatory organisms. In spite of the extreme conditions, these systems have well developed biogeochernical cycles and are extremely biologically active. The systems are generally driven by photosynthetic organisms, such as cyanobacteria. which fix C02 and N2, and do not require external input of organic matter. A complex community of both aerobic and anaerobic bacteria develop around the primary production of the cyanobacteria. Some of the constituent members of the microbial community are metabolically versatile, utilizing a variety of electron donors and electron acceptors. ~&crobial mats have been implicated in promoting the rapid degradation of crude oil, most likely due to the overall metabolic diversity of the community. This study focuses on hypersaline marine microbial mats from Solar Lake, Egypt. The Solar Lake microbial mats have been characterized by extensive biological, chemical and physical examination. During the diumal cycle, the surface layers of the mat undergo significant changes in physical and chemical conditions. These transient conditions include changing oxygen concentrations (from 0 to > 1000 micromolar), sulfide concentrations (0 to > 500 micromolar), pH (from neutral to >9.5), temperature, organic carbon (in quantity and type), among others. Tbe high photosynthetic activity of the cyanobacteria creates a situation during the day in which the surface layers (0-2.5 mm) are oxygenated, often in excess of saturation. However, during the night, diffusion from the overlying water column is the only source of oxygen, and the system becomes anaerobic at a depth of 0.5 mm. Oxygen is consumed at all times by a variety of heterotrophic and lithotrophic organisms, causing rapid depletion of oxygen below regions of photosynthetic production or rapid diffusion. Below these oxygenated regions, sulfide concentrations, due to the activity of the sulfate reducing bacteria (SRB), increase rapidly. Nficrobial populations may respond to these environmental changes by altering their metabolism or by relocating to more favorable position in the mat. Nficrocoleus chtonoplastes, predominant microbial mat cyanobacteria, have been observed to undergo migratory behavior in response to changing light conditions. These bacteria produce large sheath tubes (identified in previous microscopy) which penetrate the mat vertically, and they may migrate inside these sheaths. Theoretically the sheaths may also be utilized by other bacteria, although previous microscopy did not identify other organisms inside the sheaths. One of the main elements of this research is to link mat physical structure with mat function, and in particular, migration of mat microorganisms and transport of pollutants. One aspect of this is to characterize the physical and biology'structure of the microbial mat matrix without modification due to fixing. Previous microscopy of the mat employed fixing procedures using gluteraldehyde, as well as ethanol and propylene oxide for dehydration. We are interested in employing rapid freezing techniques to preserve our sample with a minimum of alteration. Of particular concern is preservation of the polysaccharide matrix of the mat. The mat has a thick and rubbery texture (especially the surface layer) due to the copious production of polysaccharides by mat bacteria. Overall, we would be most interested in examine the structure of the top 4 mm of the mat. In addition to being the most biologically active region of the mat, we also have a significant amount of population data for this region, at extremely high resolution (50 microme-ter vertical sections.) We are interested in looking at the overall structure and at the dimensions of the pore spaces in the mat matrix. Open spaces, in addition to the sheath tubes, may serve as conduits for migration of mat microbiota and for transport of pollutants. Specifically, we would like to look at the mat matrix in two dimensions: vertically, to look a the change in texture with depth, and horizontally, to assess heterogeneity in the mat matrix at a single depth.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Biotechnology Resource Grants (P41)
Project #
3P41RR000570-28S1
Application #
6117338
Study Section
Project Start
1998-09-30
Project End
2000-06-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
28
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Type
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Mavroudi, Maria; Zarogoulidis, Paul; Porpodis, Konstantinos et al. (2014) Stem cells' guided gene therapy of cancer: New frontier in personalized and targeted therapy. J Cancer Res Ther (Manch) 2:22-33
Malecki, Marek; Putzer, Emily; Sabo, Chelsea et al. (2014) Directed cardiomyogenesis of autologous human induced pluripotent stem cells recruited to infarcted myocardium with bioengineered antibodies. Mol Cell Ther 2:
Malecki, Marek (2014) 'Above all, do no harm': safeguarding pluripotent stem cell therapy against iatrogenic tumorigenesis. Stem Cell Res Ther 5:73
Malecki, Marek; LaVanne, Christine; Alhambra, Dominique et al. (2013) Safeguarding Stem Cell-Based Regenerative Therapy against Iatrogenic Cancerogenesis: Transgenic Expression of DNASE1, DNASE1L3, DNASE2, DFFB Controlled By POLA1 Promoter in Proliferating and Directed Differentiation Resisting Human Autologous Pluripotent J Stem Cell Res Ther Suppl 9:
Malecki, Marek; Tombokan, Xenia; Anderson, Mark et al. (2013) TRA-1-60(+), SSEA-4(+), POU5F1(+), SOX2(+), NANOG(+) Clones of Pluripotent Stem Cells in the Embryonal Carcinomas of the Testes. J Stem Cell Res Ther 3:
Malecki, Marek (2013) Improved targeting and enhanced retention of the human, autologous, fibroblast-derived, induced, pluripotent stem cells to the sarcomeres of the infarcted myocardium with the aid of the bioengineered, heterospecific, tetravalent antibodies. J Stem Cell Res Ther 3:
Malecki, Marek; Dahlke, Jessica; Haig, Melissa et al. (2013) Eradication of Human Ovarian Cancer Cells by Transgenic Expression of Recombinant DNASE1, DNASE1L3, DNASE2, and DFFB Controlled by EGFR Promoter: Novel Strategy for Targeted Therapy of Cancer. J Genet Syndr Gene Ther 4:152
Zarogoulidis, Paul; Darwiche, Kaid; Sakkas, Antonios et al. (2013) Suicide Gene Therapy for Cancer - Current Strategies. J Genet Syndr Gene Ther 4:
Malecki, Marek; Sabo, Chelsea; Putzer, Emily et al. (2013) Recruitment and retention of human autologous CD34+ CD117+ CD133+ bone marrow stem cells to infarcted myocardium followed by directed vasculogenesis: Novel strategy for cardiac regeneration. Mol Cell Ther 1:
Malecki, Marek; Malecki, Bianca (2012) Routing of Biomolecules and Transgenes' Vectors in Nuclei of Oocytes. J Fertili In Vitro 2012:108-118

Showing the most recent 10 out of 24 publications