Kasumi Masuda scite author profile

Although several risk factors for stroke have been identified, one-third remain unexplained. Here we show that infection with Streptococcus mutans expressing collagen-binding protein (CBP) is a potential risk factor for haemorrhagic stroke. Infection with serotype k S. mutans, but not a standard strain, aggravates cerebral haemorrhage in mice. Serotype k S. mutans accumulates in the damaged, but not the contralateral hemisphere, indicating an interaction of bacteria with injured blood vessels. The most important factor for high-virulence is expression of CBP, which is a common property of most serotype k strains. The detection frequency of CBP-expressing S. mutans in haemorrhagic stroke patients is significantly higher than in control subjects. Strains isolated from haemorrhagic stroke patients aggravate haemorrhage in a mouse model, indicating that they are haemorrhagic stroke-associated. Administration of recombinant CBP causes aggravation of haemorrhage. Our data suggest that CBP of S. mutans is directly involved in haemorrhagic stroke.

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Identification and characterization of a collagen‐binding protein, Cbm, in Streptococcus mutans

Nomura

Nakano

Naka

et al. 2012

Molecular Oral Microbiology

111

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Streptococcus mutans, a major pathogen of dental caries, is occasionally isolated from the blood of patients with infective endocarditis. Bacterial attachment of exposed collagen tissue in the impaired endothelium is an important step in the onset of infective endocarditis. In our previous studies, some S. mutans strains were shown to possess collagen-binding activities and most of them had an approximately 120-kDa cell-surface collagen-binding protein called Cnm. However, several strains without Cnm proteins show collagen-binding properties. In the present study, another collagen-binding protein, Cbm, was characterized and its coding gene cbm was sequenced in these strains. The amino acid alignment in the putative collagen-binding domain of Cbm was shown to have approximately 80% identity and 90% similarity to the comparable region of Cnm. Cbm-deficient isogenic mutant strains constructed by insertional inactivation of the cbm gene, lacked collagen-binding properties, which were recovered in the complemented mutant. Analyses of a large number of clinical isolates from Japan, Thailand and Finland revealed that cbm-positive strains were present in all of these countries and that cnm-positive and cbm-positive strains were detected in the oral cavity of approximately 10 and 2% of systemically healthy subjects, respectively. In addition, cnm-positive strains were predominantly identified in the serotype f group, whereas cbm-positive strains were frequently detected in serotype k. These results suggest that Cbm as well as Cnm are major cell surface proteins of S. mutans associated with binding to type I collagen and predominantly identified in serotype k strains.

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Energy loss in the left ventricle obtained by vector flow mapping as a new quantitative measure of severity of aortic regurgitation: a combined experimental and clinical study

et al. 2015

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Assessment of Myocardial Ischemic Memory Using Speckle Tracking Echocardiography

Asanuma

Fukuta

Masuda

et al. 2012

JACC: Cardiovascular Imaging

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Assessment of Myocardial Ischemic Memory Using Persistence of Post-Systolic Thickening After Recovery From Ischemia

Asanuma

Uranishi

Masuda

et al. 2009

JACC: Cardiovascular Imaging

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Colour doppler sonography of breast masses: A multiparameter analysis

Buadu¹,

Murakami²,

Murayama³

et al. 1997

Clinical Radiology

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Metal ion and vitamin adsorption profiles of phosphate binder ion-exchange resins

Takagi¹,

Masuda²,

Yamazaki³

et al. 2010

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Solid-state 13C NMR study of indomethacin polymorphism

Masuda

Tabata

Kono³

et al. 2006

International Journal of Pharmaceutics

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Kasumi Masuda

The collagen-binding protein of Streptococcus mutans is involved in haemorrhagic stroke

Identification and characterization of a collagen‐binding protein, Cbm, in Streptococcus mutans

Energy loss in the left ventricle obtained by vector flow mapping as a new quantitative measure of severity of aortic regurgitation: a combined experimental and clinical study

Assessment of Myocardial Ischemic Memory Using Speckle Tracking Echocardiography

Assessment of Myocardial Ischemic Memory Using Persistence of Post-Systolic Thickening After Recovery From Ischemia

Colour doppler sonography of breast masses: A multiparameter analysis

Metal ion and vitamin adsorption profiles of phosphate binder ion-exchange resins

Solid-state 13C NMR study of indomethacin polymorphism

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