Abstract

The long term objectives of this program are to define, at molecular and cellular levels, interactions between bacteria and mammalian cells. The focus is on: (1) Biochemical changes phagocytic leukocytes undergo when they ingest a bacterium (or are otherwise stimulated) - insofar as these changes are part of the leukocyte's anti-bacterial armamentarium; (ii) The effect on the host organism's cells of substances released as a result of phagocytic killing and dismantling of the bacterium. In the first context, release of active oxygen radicals by phagocytic leukocytes is the main focus, and is in the mainstream of studies of control of infection. In the second context the focus is on the effect on mammalian cells of muramyl peptides (components of the bacterial cell wall) that are released from engulfed bacteria (and also by enzyme action on dead bacteria of the gut). The latter substances are known to stimulate the host immune system. They also are fever-inducing. Finally, they are somnogenic (i.e., promote slow-wave sleep). The last mentioned consideration is neglected in the mainstream of investigations of infection. Experiments to achieve the goals outlined consist in isolating appropriate mammalian cells, and in the first context, stimulating them in a variety of ways while following release of superoxide and monitoring other cellular, especially membrane, functions. In the second category, the questions have developed into considerations of the mechanism(s) by which muramyl peptides induce physiological changes in mammalian cells - i.e., the matter has progressed from the """"""""whole-animal"""""""" effect (e.g., slow- wave sleep induction) to the cellular level - in particular, studies of specific cellular binding sites (receptors?) for muramyl peptides and sequels of binding. A key matter is that muramyl peptides (immunostimulants) and serotonin (a neuro- transmitter) compete for the same cellular binding sites, and induce several responses in common. In addition, B-lymphocytes of narcoleptics (who have a derangement of normal sleep) do not bind muramyl peptides in contradistinction to cells of normals. Since narcolepsy is characterized by a specific immune situation (expression of histocompatibility antigen DR2, DQwl) this constitutes a further link between the immune and neurological systems. These matters are health-related in that they deal with the host's antimicrobial mechanisms, and with secondary effects of bacterial death, i.e., neuro-immune interactions due to bacterial breakdown products.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI003260-32
Application #
3124130
Study Section
Bacteriology and Mycology Subcommittee 2 (BM)
Project Start
1978-01-01
Project End
1992-12-31
Budget Start
1991-01-01
Budget End
1992-12-31
Support Year
32
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Type
Schools of Medicine
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Polanski, M; Vermeulen, M W; Wu, J et al. (1995) Muramyl dipeptide mimicry in the regulation of murine macrophage activation by serotonin. Int J Immunopharmacol 17:225-32
Camarero, V C; Colepicolo, P; Ribeiro, J M et al. (1993) Leukocyte-deactivating factor from macrophages: partial purification and biochemical characterization. A novel cytokine. J Cell Physiol 157:84-9
Polanski, M; Karnovsky, M L (1992) Serotonergic aspects of the response of human platelets to immune-adjuvant muramyl dipeptide. J Neuroimmunol 37:149-60
Karnovsky, M L (1991) Role of biological membranes in slow-wave sleep. J Bioenerg Biomembr 23:123-32
Camarero, V C; Junqueira, V B; Colepicolo, P et al. (1990) Epithelial macrophages secrete a deactivating factor for superoxide release. J Cell Physiol 145:481-7
Colepicolo, P; Camarero, V C; Nicolas, M T et al. (1990) A sensitive and specific assay for superoxide anion released by neutrophils or macrophages based on bioluminescence of polynoidin. Anal Biochem 184:369-74
Silverman, D H; Sayegh, M H; Alvarez, C E et al. (1990) HLA class II-restricted binding of muramyl peptides to B lymphocytes of normal and narcoleptic subjects. Hum Immunol 27:145-54
Silverman, D H; Imam, K; Karnovsky, M L (1989) Muramyl peptide/serotonin receptors in brain-derived preparations. Pept Res 2:338-44
Heyworth, P G; Karnovsky, M L; Badwey, J A (1989) Protein phosphorylation associated with synergistic stimulation of neutrophils. J Biol Chem 264:14935-9
Silverman, D H; Karnovsky, M L (1989) Serotonin and peptide immunoneuromodulators: recent discoveries and new ideas. Adv Enzymol Relat Areas Mol Biol 62:203-26

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