22 research outputs found
Genome-Based Analysis of Heme Biosynthesis and Uptake in Prokaryotic Systems
No full textHeme is the prosthetic group of many proteins that carry out a variety of key biological functions. In addition, for many pathogenic organisms, heme (acquired from the host) may constitute a very important source of iron. Organisms can meet their heme demands by taking it up from external sources, by producing the cofactor through a dedicated biosynthetic pathway, or both. Here we analyzed the distribution of proteins specifically involved in the processes of heme biosynthesis and heme uptake in 474 prokaryotic organisms. These data allowed us to identify which organisms are capable of performing none, one, or both processes, based on the similarity to known systems. Some specific instances where one or more proteins along the pathways had unusual modifications were singled out. For two key protein domains involved in heme uptake, we could build a series of structural models, which suggested possible alternative modes of heme binding. Future directions for experimental work are given
Genome-Based Analysis of Heme Biosynthesis and Uptake in Prokaryotic Systems
No full textHeme is the prosthetic group of many proteins that carry out a variety of key biological functions. In addition, for many pathogenic organisms, heme (acquired from the host) may constitute a very important source of iron. Organisms can meet their heme demands by taking it up from external sources, by producing the cofactor through a dedicated biosynthetic pathway, or both. Here we analyzed the distribution of proteins specifically involved in the processes of heme biosynthesis and heme uptake in 474 prokaryotic organisms. These data allowed us to identify which organisms are capable of performing none, one, or both processes, based on the similarity to known systems. Some specific instances where one or more proteins along the pathways had unusual modifications were singled out. For two key protein domains involved in heme uptake, we could build a series of structural models, which suggested possible alternative modes of heme binding. Future directions for experimental work are given
Genome-Based Analysis of Heme Biosynthesis and Uptake in Prokaryotic Systems
No full textHeme is the prosthetic group of many proteins that carry out a variety of key biological functions. In addition, for many pathogenic organisms, heme (acquired from the host) may constitute a very important source of iron. Organisms can meet their heme demands by taking it up from external sources, by producing the cofactor through a dedicated biosynthetic pathway, or both. Here we analyzed the distribution of proteins specifically involved in the processes of heme biosynthesis and heme uptake in 474 prokaryotic organisms. These data allowed us to identify which organisms are capable of performing none, one, or both processes, based on the similarity to known systems. Some specific instances where one or more proteins along the pathways had unusual modifications were singled out. For two key protein domains involved in heme uptake, we could build a series of structural models, which suggested possible alternative modes of heme binding. Future directions for experimental work are given
Genome-Based Analysis of Heme Biosynthesis and Uptake in Prokaryotic Systems
No full textHeme is the prosthetic group of many proteins that carry out a variety of key biological functions. In addition, for many pathogenic organisms, heme (acquired from the host) may constitute a very important source of iron. Organisms can meet their heme demands by taking it up from external sources, by producing the cofactor through a dedicated biosynthetic pathway, or both. Here we analyzed the distribution of proteins specifically involved in the processes of heme biosynthesis and heme uptake in 474 prokaryotic organisms. These data allowed us to identify which organisms are capable of performing none, one, or both processes, based on the similarity to known systems. Some specific instances where one or more proteins along the pathways had unusual modifications were singled out. For two key protein domains involved in heme uptake, we could build a series of structural models, which suggested possible alternative modes of heme binding. Future directions for experimental work are given
MetalS<sup>2</sup>: A Tool for the Structural Alignment of Minimal Functional Sites in Metal-Binding Proteins and Nucleic Acids
No full textWe
developed a new software tool, MetalS<sup>2</sup>, for the structural
alignment of Minimal Functional Sites (MFSs) in metal-binding biological
macromolecules. MFSs are 3D templates that describe the local environment
around the metal(s) independently of the larger context of the macromolecular
structure. Such local environment has a determinant role in tuning
the chemical reactivity of the metal, ultimately contributing to the
functional properties of the whole system. On our example data sets,
MetalS<sup>2</sup> unveiled structural similarities that other programs
for protein structure comparison do not consistently point out and
overall identified a larger number of structurally similar MFSs. MetalS<sup>2</sup> supports the comparison of MFSs harboring different metals
and/or with different nuclearity and is available both as a stand-alone
program and a Web tool (http://metalweb.cerm.unifi.it/tools/metals2/)
