Abstract

The key metalloprotein of dissimilator nitrite reductase found in the majority of microbial denitrifiers is called cytochrome cd which contains an extractable green heme prosthetic group. This so-called -d-l heme has been assumed to be a chlorin since the late 1950's. Recently a structure determination of isolated heme -d-l by another laboratory also favored a chlorin macrocycle. However, critical analyses of the available spectra data have led us to propose that the -d-1 heme is not a chlorin but a dioxoisobacteriochlorin. Recent experimental studies on demetalated heme -d-1 and model compounds have yielded convincing evidence to support the novel dioxo ring structure. The objectives of the proposed research are (1) to establish unambiguously the structure of the -d-1 heme; (2) to elucidate the intrinsic physicochemical properties of this ring and to identify the attributes which make this heme uniquely suitable for mediating the nitrite reduction; and (3) to understand the reaction pathways and mechanisms. Our experimental approach includes (1) chemical derivatizations of isolated -d-1 for further confirmation of the proposed structure; (2) study of new synthetic methods to prepare dioxoisobacteriochlorins as models and analogues for -d-1 and ultimately, the total synthesis of -d-1; (3) systematic study and documentation of the spectroscopic properties and ligand coordination chemistry of heme -d-1 and model compounds to provide a knowledge base for this class of heme groups; (4) the substitution of synthetic metal dioxo-isobacteriochlorin complexes into the active sites of myoglobin and cytochrome cd to probe the structural basis of prosthetic group/protein interactions; and (5) tests of possible reduction pathways for dioxygen and nitrite reductions using heme models and reconstituted proteins. Denitrification is a basic energy coupled process of metabolism in a large variety of bacteria, including some pathogens. Furthermore, products of denitrification are NO-2-.NO and N20, all of which have direct or indirect toxicity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM036520-01
Application #
3290636
Study Section
Metallobiochemistry Study Section (BMT)
Project Start
1986-04-01
Project End
1989-03-31
Budget Start
1986-04-01
Budget End
1987-03-31
Support Year
1
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Michigan State University
Department
Type
Schools of Arts and Sciences
DUNS #
193247145
City
East Lansing
State
MI
Country
United States
Zip Code
48824

  Publications

Chang, C K (1994) Haem d1 and other haem cofactors from bacteria. Ciba Found Symp 180:228-38;discussion 238-46
Weeg-Aerssens, E; Wu, W S; Ye, R W et al. (1991) Purification of cytochrome cd1 nitrite reductase from Pseudomonas stutzeri JM300 and reconstitution with native and synthetic heme d1. J Biol Chem 266:7496-502
Andersson, L A; Loehr, T M; Wu, W S et al. (1990) Modelling heme d1. The spectral properties of copper(II) porphyrindiones. FEBS Lett 267:285-8
Salehi, A; Oertling, W A; Fonda, H N et al. (1988) Resonance Raman spectra of the II-cation radicals of copper, cobalt, and nickel methyloctaethylchlorins: vibrational characteristics of chlorophyll models. Photochem Photobiol 48:525-30
Chang, C K; Timkovich, R; Wu, W (1986) Evidence that heme d1 is a 1,3-porphyrindione. Biochemistry 25:8447-53