Nonspecific resistance to Escherichia coli in mice

Shayegani, Mehdi; Parsons, L M

doi:10.1128/iai.12.4.779-784.1975

Cited by 3 publications

(1 citation statement)

References 12 publications

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“…Cell wall mucopeptide (peptidoglycan or murein) from S. aureus Cowan I was prepared as described by Shayegani et al [24]. Cell walls obtained after disintegration of bacteria with a Braun homogenizer were thoroughly washed and digested with trypsin.…”

Section: Cell Wall Fractions Of S Aureusmentioning

confidence: 99%

Lymphocyte stimulation by protein A of Staphylococcus aureus

1976

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Protein A from Staphylococcus aureus (SpA) is known to bind to the Fc region of most mammalian IgG classes. In the present article data are presented showing that SpA is a highly efficient mitogen for human peripheral B lymphocytes, with no detectable activity for T lymphocytes. In order to achieve optimal stimulating conditions SpA should be presented to the lymphocytes on an insoluble matrix, such as the SpA-positive bacteria themselves or SpA covalently attached to Sephadex or Sepharose beads. Using such conditions SpA is equivalent with regard to stimulatory capacity for B lymphocytes as phytohemagglutinin is for the human T lymphocytes. Specificity controls proved beyond doubt that SpA and not any other contaminating product is the B cell mitogen. It is concluded that SpA as an inducer of human B lymphocyte division might serve as a highly useful assay in the clinical assessment of B lymphocyte function. It should also be a suitable tool in the fine analysis of B lymphocyte activation via the specific interactions with surface IgG molecules.

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Section: Cell Wall Fractions Of S Aureusmentioning

confidence: 99%

Lymphocyte stimulation by protein A of Staphylococcus aureus

1976

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Staphage lysate: an immunomodulator of the primary immune response in mice

Esber¹,

Ganfield²,

Rosenkrantz³

1985

Immunopharmacology

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Specific and Nonspecific Immune Resistance Enhancing Activity of Staphage Lysate

Esber¹,

DeCourcy²,

Bogdén³

1981

Journal of Immunopharmacology

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The immunopotentiating activity of staphage lysate (SPL) was evaluated in terms of its immune protection against lethal bacterial infection and its antitumor activity. Mice were pretreated weekly with 10(8) viable, Staphylococcus aureus, strain 18Z for 3 weeks (Induction), followed by intraperitoneal SPL injections (Elicitation) at various times in relation to infectious challenge or tumor implantation. Induction without elicitation, or elicitation alone failed to provide protection against Klebsiella pneumoniae infection and resulted in only 30-40% survival against homologous infection with pathogenic S. aureus type III, whereas combined induction and elicitation produced enhanced resistance induction and elicitation regimens resulted in 50% and 80-100% survival in mice inoculated with K. pneumoniae and S. aureus, respectively. SPL had no antitumor effect in mice implanted with median survival time resulting from induction and elicitation in animals implanted which Ehrlich's ascites. This enhancement of immune resistance may possibly be related to activation of thymus-modulated lymphocytes and macrophages by SPL.

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Nonspecific resistance to Escherichia coli in mice

Cited by 3 publications

References 12 publications

Lymphocyte stimulation by protein A of Staphylococcus aureus

Lymphocyte stimulation by protein A of Staphylococcus aureus

Staphage lysate: an immunomodulator of the primary immune response in mice

Specific and Nonspecific Immune Resistance Enhancing Activity of Staphage Lysate

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