Identification of a haem-utilization protein (Hup) in Haemophilus influenzae

Morton, Daniel J.; Smith, Ann; Ren, Zhen; Madore, Larissa L.; VanWagoner, Timothy M.; Seale, Thomas W.; Whitby, Paul W.; Stull, Terrence L.

doi:10.1099/mic.0.27238-0

Cited by 48 publications

(68 citation statements)

References 53 publications

(37 reference statements)

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“…Stock solutions were prepared as previously described [9,10]. Rabbit hemopexin was prepared as described previously [11].…”

Section: Heme Sourcesmentioning

confidence: 99%

“…Primers were designated eP4-1 (5′-ATACCCTGAATGAATAGG-3′) and eP4-2 (5′-AAATCGATCTTTTTAATGG-3′). PCRs were performed as previously described [11] using an annealing temperature of 51°C. Products were successfully cloned into the TA cloning vector pCR2.1-TOPO and confirmed by DNA sequencing.…”

Section: Construction Of Hel Mutantsmentioning

confidence: 99%

“…A rat model was used to assess bacteremia in both 5-day old and 30-day old rats as previously described [10,11,14]. Specified pathogen free timed-pregnant Sprague-Dawley rats were received five days prior to parturition.…”

Section: Animal Modelmentioning

confidence: 99%

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Lipoprotein e (P4) of Haemophilus influenzae: role in heme utilization and pathogenesis

Morton

Smith

VanWagoner

et al. 2007

Microbes and Infection

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Lipoprotein e (P4) of Haemophilus influenzae is a phosphomonoesterase, encoded by the hel gene, that has been implicated in the acquisition of heme by this fastidious organism. However, lipoprotein e (P4) is also involved in the utilization of NAD and NMN. Some reports have concluded that the reported heme-related growth defect actually reflects a growth defect for NAD. In the current study hel insertion mutants were constructed and a role for e (P4) in heme acquisition was demonstrated independent of its role in NAD or NMN acquisition. In addition a rat model of infection demonstrated a role for e (P4) in the pathogenesis of invasive disease.

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“…Stock solutions were prepared as previously described [9,10]. Rabbit hemopexin was prepared as described previously [11].…”

Section: Heme Sourcesmentioning

confidence: 99%

Section: Construction Of Hel Mutantsmentioning

confidence: 99%

See 1 more Smart Citation

Lipoprotein e (P4) of Haemophilus influenzae: role in heme utilization and pathogenesis

Morton

Smith

VanWagoner

et al. 2007

Microbes and Infection

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“…Four separate pairs of primers (Table 2) were designed for use in the PCR based on the Rd KW20 genomic sequence. The PCRs were performed in a 50 ml reaction as previously described (Morton et al, 2004b) except that annealing temperatures and extension times were as below. HXUCUSA and HXUCUSB were used to amplify an~1100 bp fragment upstream of hxuC (annealing temperature 56 uC, extension time 1 min); HXUC-A and HXUC-B to amplify an~2500 bp fragment encompassing the entire coding sequnce of hxuC (annealing temperature 58 uC, extension time 2 min 40 s); HXUCDSA and HXUBDSB to amplify an~2800 bp fragment including the entire coding sequence of hxuB and part of hxuA (annealing temperature 56 uC, extension time 3 min); and HXUBDSA and HXUADSB to amplify añ 3800 bp fragment including the entire coding sequence of hxuA and~1000 bp downstream of hxuA (annealing temperature 60 uC, extension time 4 min).…”

Section: Methodsmentioning

confidence: 99%

“…Haem-deplete growth was performed in BHI broth supplemented with only 10 mg b-NAD ml 21 (haemdeplete BHI; hdBHI). H. influenzae were transformed to antibiotic resistance using a modification of the static aerobic method of Gromkova et al (1989) as previously described (Morton et al, 2004b).…”

Section: Methodsmentioning

confidence: 99%

The haem–haemopexin utilization gene cluster (hxuCBA) as a virulence factor of Haemophilus influenzae

et al. 2007

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Haemophilus influenzae has an absolute growth requirement for a porphyrin source, which can be supplied in vitro by haem, haemoglobin, or the haemoglobin-haptoglobin, haem-haemopexin and haem-albumin complexes. Utilization of the haem-haemopexin complex is known to be mediated by the products of the hxuCBA gene cluster. It was demonstrated that hxuC, but not hxuA or hxuB, is also essential for the utilization of haem from haem-albumin complexes. Mutants of the type b strain E1a lacking genes in the hxuCBA gene cluster were examined for their ability to cause bacteraemia in rat models of invasive disease. In 5-day-old rats, mutants in the hxuCBA genes yielded a significantly reduced bacteraemic titre compared to the wild-type strain. In addition, 5-day-old rats infected with the hxuCBA mutant strains exhibited significantly improved survival rates compared to those infected with the wild-type strain. Mutations in the haemoglobin/haemoglobinhaptoglobin-binding protein genes (hgps), either alone or in combination with the hxuCBA mutations, had no impact on virulence in 5-day-old rats. In 30-day-old rats infected with either the hxuCBA mutants or the wild-type strains, there was no significant difference in the ability to establish bacteraemia although bacterial titres were lower in rats infected with the hxuCBA mutants than in those infected with the wild-type strain. These age-related differences in the impact of mutations in the hxuCBA gene cluster may be related to changes in levels of host haem-binding proteins during development of the rat.

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Covalent bonding of heme to protein prevents heme capture by nontypeable Haemophilus influenzae

et al. 2017

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Nontypeable Haemophilus influenzae (NTHi) are Gram‐negative pathogens that contribute to a variety of diseases, including acute otitis media and chronic obstructive pulmonary disease. As NTHi have an absolute requirement for heme during aerobic growth, these bacteria have to scavenge heme from their human hosts. These heme sources can range from free heme to heme bound to proteins, such as hemoglobin. To test the impact of heme structural factors on heme acquisition by NTHi, we prepared a series of heme sources that systematically vary in heme exposure and covalent binding of heme to peptide/protein and tested the ability of NTHi to use these sources to support growth. Results from this study suggest that NTHi can utilize protein‐associated heme only if it is noncovalently attached to the protein.

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Identification of a haem-utilization protein (Hup) in Haemophilus influenzae

Cited by 48 publications

References 53 publications

Lipoprotein e (P4) of Haemophilus influenzae: role in heme utilization and pathogenesis

Lipoprotein e (P4) of Haemophilus influenzae: role in heme utilization and pathogenesis

The haem–haemopexin utilization gene cluster (hxuCBA) as a virulence factor of Haemophilus influenzae

Covalent bonding of heme to protein prevents heme capture by nontypeable Haemophilus influenzae

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