Bordetella pertussis: Difference between revisions

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Classification

Klebsiella pnemoniae
Scientific classification
Kingdom: Eubacteria Phylum: Proteobacteria Class: Gamma Proteobacteria Order: Pseudomonadales Family: Pseudomonadaceae Genus: Pseudomonas Species: putida
Binomial name
Pseudomonas putida

Kingdom: Bacteria

Phylum: Proteobacteria

Class: Betaproteobacteria

Order: Burkholderiales

Family: Alcaligenaceae

Genus: Bordetella

Species: B. pertussis

Description and Significance

Bordetella pertusis, commonly known as whooping cough, was first defined in the 16th century. It is a respiratory tract infection depicted by a paroxysmal cough. Bordetella pertusis is extremely tiny, and is a Gram-negative aerobic coccobacilius. It can appear in singles or in pairs. Before vaccinations were prevalent, Bordetella pertusis was a major cause of death among children and infants. After the pertusis vaccine was introduced, reported cases of this infection decreased by more than 99%. Even though this infection has been contained for the most part, it is still remains a disease that is of major concern.

Ecology

Humans are the only home for Bordetella pertusis. Through aerosolized droplets from coughing, Bordetella pertusis is spread. The pathogen is contagious and can be transferred from person to person through these droplets by sneezing or coughing. This gram-negative pleomorphic bacillius attaches to and damages ciliated respiratory epithelium. Its main residence is within the trachea and the bronchi. The pathogen will cease to exist in the environment if it is not embedded in the respiratory mucus of the host.

Genome Structure

Tomaha I, a strain of Bordetella pertusis has its genome completely sequenced. One circular chromosome containing 4.086,189 nucleotides. GC bonds makes up approximately 67% of the genome. The coding density is 82%.

Another genome that is also sequenced from Bordetella pertusis is IncP-1 beta plasmid pBP135. 41,268 base pair nucleotides are contained in this genome. It also carries 46 ORF's. Two of these ORF's have closely resemble genes from a plant pathogen called "Xylella fastidiosa". These genes functions are unknown.

Cell Structure and metabolism

Being an aerobe, Bordetella pertusis uses aerobic respiration as its metabolism. Its cell structure consists of an inner membrane, outer membrane, and periplasmic space. The periplasmic space contains a thin peptidoglycan wall layer in between it. Lipopolysaccharides reside on the outer membrane. These types of endotoxins are not seen in any other Gram-negative bacteria. The lipopolysaccharides in Bordetella pertusis contain two forms, which differ in there phosphate composition of the lipid region of the lipopolysaccharide. Lipid X is the designation of this unusual lipid, which is usually in the Lipid A form. Lipid X's function is not known.

Pathology

Humans are the only home for Bordetella pertusis. The respiratory disease caused by Bordetella pertusis is known as pertussis. It is highly contagious, especially in the early stages, and consists of violent coughing which is immediately followed by "whooping" sounds during the intake air. Hence, this disease also known as "Whooping Cough". Vomiting is also a symptom of this disease. It also consists of discharge which contain sticky mucus. Other symptoms of pertussis are runny nose, coughing sneezing, and a minor fever.

The whooping cough is due to one of the virulence factors of Bordetella pertusis, adenylate cyclase toxin. (CyaA) CyaA is a single polypeptide which attacks eukaryotic cells by directly moving across the plasma membrane of the target cell. It helps in the initiation of the infection by reducing phagocytic activity. CyaA contains two domains. An enzymatic domain and a binding domain, which attaches itself to the surface of the hosts cells. CyaA is only active when calmodulin, a eukaryotic regulatory molecule, is present. Therefore it is not present in prokaryotes. Pertussis toxin is another major virulence factor of Bordetella pertusis. It is a major factor of the respiratory infection, especially in the early stages. Pertussis toxins' main target are the macrophages in the respiratory tract. By doing so, pertussis toxin is able to promote the infection. Another virulence factor Bordetella pertusis that is responsible for cell adhesion to host cells is filamentous hemagglutinin.

Frequency

 Bordetella pertusis occurs mostly during the summer months, usually occurring between June and September.  Lifelong immunity is not attained, even if an individual is vaccinated or has even acquired the disease once before.  The vaccination usually lasts about three to five years.   Bordetella pertusis infects people of every age, but infants are more susceptible than any other group.