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A minimal gene set for cellular life derived by comparison of complete bacterial genomes

TLDR
Fraser et al. as mentioned in this paper compared the 468 predicted M. genitalium protein sequences with the 1703 protein sequences encoded by the other completely sequenced small bacterial genome, that of Haemophilus influenzae, and suggested that the remaining 256 genes are close to the minimal gene set that is necessary and sufficient to sustain the existence of a modern type cell.
Abstract
The recently sequenced genome of the parasitic bacterium Mycoplasma genitalium contains only 468 identified protein-coding genes that have been dubbed a minimal gene complement [Fraser, C.M., Gocayne, J.D., White, O., Adams, M.D., Clayton, R.A., et al. (1995) Science 270, 397-403]. Although the M. genitalium gene complement is indeed the smallest among known cellular life forms, there is no evidence that it is the minimal self-sufficient gene set. To derive such a set, we compared the 468 predicted M. genitalium protein sequences with the 1703 protein sequences encoded by the other completely sequenced small bacterial genome, that of Haemophilus influenzae. M. genitalium and H. influenzae belong to two ancient bacterial lineages, i.e., Gram-positive and Gram-negative bacteria, respectively. Therefore, the genes that are conserved in these two bacteria are almost certainly essential for cellular function. It is this category of genes that is most likely to approximate the minimal gene set. We found that 240 M. genitalium genes have orthologs among the genes of H. influenzae. This collection of genes falls short of comprising the minimal set as some enzymes responsible for intermediate steps in essential pathways are missing. The apparent reason for this is the phenomenon that we call nonorthologous gene displacement when the same function is fulfilled by nonorthologous proteins in two organisms. We identified 22 nonorthologous displacements and supplemented the set of orthologs with the respective M. genitalium genes. After examining the resulting list of 262 genes for possible functional redundancy and for the presence of apparently parasite-specific genes, 6 genes were removed. We suggest that the remaining 256 genes are close to the minimal gene set that is necessary and sufficient to sustain the existence of a modern-type cell. Most of the proteins encoded by the genes from the minimal set have eukaryotic or archaeal homologs but seven key proteins of DNA replication do not. We speculate that the last common ancestor of the three primary kingdoms had an RNA genome. Possibilities are explored to further reduce the minimal set to model a primitive cell that might have existed at a very early stage of life evolution.

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Comparative analysis of essential genes in prokaryotic genomic islands.

TL;DR: It is concluded that essential genes in GIs are significantly fewer than those outside GIs and this will shed new light on the development of the prediction algorithm of essential genes, but also give a clue to detect the functionality ofessential genes in genomic islands.
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Harnessing model organism genomics to underpin the machine learning-based prediction of essential genes in eukaryotes - Biotechnological implications.

TL;DR: An historical review of experimental and computational approaches employed for the characterisation of essential genes in eukaryotes is undertaken, with a particular focus on model ecdysozoans (C. elegans and D. melanogaster), and the possible applicability of ML-approaches to organisms such as socioeconomically important parasites is discussed.
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Backbone and sidechain 1H, 13C and 15N chemical shift assignments of the hydrophobin DewA from Aspergillus nidulans

TL;DR: The backbone and sidechain assignments for the class I hydrophobin DewA from the fungus Aspergillus nidulans are reported, showing the formation of coatings on fungal structures to render them hydrophobic.
Journal ArticleDOI

Small genomes and the difficulty to define minimal translation and metabolic machineries

TL;DR: This work discusses the state-of-the-art of the definition of the minimal genome, based on current knowledge about bacteria with naturally reduced genomes, including both endosymbionts and free-living cells, and proposes a hierarchy of minimal cells supported by different metabolic networks with a complexity inversely correlated with the chemical complexity of the environment.
Journal ArticleDOI

Symbiogenesis as a Model for Reconstructing the Early Stages of Genome Evolution

TL;DR: Higher evolutionary conservation of template biosynthetic processes with respect to step processes determining the metabolism and development in cells does not support the hypothesis about emergence of genomes within the ancestral cellular metabolic systems which are thought to be of abiogenic origin, instead suggesting dualistic origin of life on Earth.
References
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Book

Bergey's Manual of Systematic Bacteriology

TL;DR: BCL3 and Sheehy cite Bergey's manual of determinative bacteriology of which systematic bacteriology, first edition, is an expansion.
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