The two studies are reported by Joseph Heitman and colleagues at Duke University Medical Center and by Fritz Mühlschlegel of the University of Kent, Jochen Buck at Cornell University, and their collaborators.
How organisms sense and respond to CO2 at the cellular level is not fully understood, but it is of great importance in understanding the biology of microbes, plants, and animals alike. For example, CO2 levels govern the detection of prey by female mosquitoes, control respiration in mammals, and of course play a critical regulatory role in photosynthesis in algae and plants; in addition, CO2 sensing and transport are involved in many cellular processes and virulence attributes of diverse pathogenic bacteria and fungi--in both B. anthracis, which causes Anthrax, and C. neoformans, which causes meningitis, CO2 induces the production of sugar-based capsules that surround and protect the invading cell from the host during infection.
In their new work, Mühlschlagel and colleagues studied the function of CO2 sensing in two major human fungal pathogens, C. albicans and C. neoformans. Both cause life-threatening, invasive infections in immunocompromised patients--for example, those infected with HIV or undergoing bone-marrow transplantation. The two fungi, which are distantly related in evolution, have different attributes governing their virulence in humans. For C. albicans, a transition between different morphological forms ("yeast" and "filamentous" forms) plays a major role, whereas for C. neoformans, synthesis of a polysaccharide capsule is key.
In the bodies of mammals, the CO2 concentration is more than 150-fold higher (5%) than it is in atmospheric air (0.033%). Consequently, C. albicans and C. neoformans are exposed to dramatically elevated CO2 concentrations when causing systemic disease. In their research, the authors identify CO2 as a physiological signal that induces the pathogenic filamentous transition in C. albicans; they also demonstrate that an ancient group of enzymes called adenylyl cyclases are the so-called chemosensors mediating both the CO2 -dependent filamentation in C. albicans and the capsule biosynthesis in C. neoformans. The authors go on to show that CO2 sensing in C. albicans is essential for superficial (skin) infections, in which yeast must be able to grow despite significantly lowered CO2 levels present at the skin surface. Based on their findings, the authors conclude that CO2 sensing is a vital mediator of fungal virulence in different host environments--for example, at different sites within the body.
In a related paper, Joseph Heitman and colleagues, also using C. neoformans as a model system for understanding fungal disease, provide new evidence that CO2 sensing and metabolism govern growth, sexual reproduction, and virulence of this pathogenic microbe.
In this work, the researchers investigated the CO2-sensing mechanism of C. neoformans. This pathogen normally infects the human host (a high-CO2 environment) from the air (low CO2) in the course of causing deadly fungal meningitis. The authors found that an enzyme called carbonic anhydrase (CA) plays a critical role in the yeast's growth in ambient air; the CA enzyme accomplishes this by providing bicarbonate substrates for fatty-acid biosynthesis and other cellular processes. In contrast, the CA enzyme is dispensible for the yeast's survival in the high- CO2 environment of the host. Another major finding of the work is that for C. neoformans, high CO2 blocks sexual differentiation, which is known to be a key process for generating infectious spores, and the CA enzyme plays a central role in the process. Together with the accompanying work by Mühlschlegel and colleagues, this study implicates a key role for CO2 in growth and differentiation in the fungal kingdom.
The identification of a link between CO2 sensing and fungal virulence may have broad implications for the study of microbial pathogens and the role of adenylyl cyclase in virulence trait regulation by CO2. Furthermore, it may in time facilitate the development of a new class of antimicrobial agents.
The researchers in the Heitman group included Yong-Sun Bahn, Gary M. Cox, John R. Perfect, and Joseph Heitman of Duke University Medical Center in Durham, North Carolina. This work was supported by NIAID R01 grants AI39115 and AI50113 to J.H. and NIAID P01 program project grant AI44975 to the Duke University Mycology Research Unit.
Bahn et al.: "Carbonic anhydrase and CO2 sensing during Cryptococcus neoformans growth, differentiation, and virulence." Publishing in Current Biology, Vol. 15, 2013-2020, November 22, 2005, DOI 10.1016/j.cub.2005.09.047, www.current-biology.com
The researchers for the Mühlschlegel/Buck group included Torsten Klengel, Wei-Jun Liang, Claudia Ruoff, Sabine E. Eckert, Estelle Gewiss Mogensen, Mick F. Tuite, and Fritz A. Mühlschlegel of the University of Kent in Kent, United Kingdom; James Chaloupka, Lonny R. Levin, and Jochen Buck of the Joan and Sanford I. Weill Medical College of Cornell University in New York; Klaus Schröppel of the Universität Erlangen in Erlangen, Germany (Present address: Robert-Bosch-Hospital in Stuttgart, Germany); Julian R. Naglik of the King's College London in London; Ken Haynes of the Imperial College London in London. This research was supported by The Wellcome Trust (to F.A.M.), BBSRC (to F.A.M.), EU (to F.A.M.), NIH (to J.B. and L.R.L.), Ellison Medical Foundation (to J.B.), and Hirschl/Weill-Caulier Foundation (to L.R.L.).
Klengel et al.: "Fungal adenylyl cyclase integrates CO2 sensing with cAMP signalling and virulence." Publishing in Current Biology, Vol. 15, 2021-2026, November 22, 2005, DOI 10.1016/j.cub.2005.10.040 www.current-biology.com