Complement activation in vivo in cancer patients receiving C. Parvum immunotherapy

H. Biran; J. L. Moake; R. C. Reed; J. U. Gutterman; E. M. Hersh; E. J. Freireich; G. M. Mavligit

doi:10.1038/bjc.1976.203

Complement activation in vivo in cancer patients receiving C. Parvum immunotherapy

H. Biran, J. L. Moake, R. C. Reed, J. U. Gutterman, E. M. Hersh, E. J. Freireich, G. M. Mavligit

Leukemia

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

Serum complement levels were assayed in 26 patients with disseminated cancer, who received immunotherapy with infusion of C. parvum. Complement activation, indicated by the consumption of C3 or C4 or both, was found in 46% of the patients. Serum samples showed direct correlation between decreased C3 and conversion of C3 proactivator, whereas such conversion did not occur when C4 alone was decreased. It is concluded that the bypass (properdin) pathway was activated in patients in whom C3 consumption was detected, while the classical (C1) pathway was activated in the patients with C4 consumption unaccompanied by C3 decrease. Direct correlation was observed between delayed cutaneous hypersensitivity reactions to recall antigens and the incidence of C. parvum-associated complement activation.

Original language	English (US)
Pages (from-to)	493-499
Number of pages	7
Journal	British journal of cancer
Volume	34
Issue number	5
DOIs	https://doi.org/10.1038/bjc.1976.203
State	Published - Nov 1976

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1038/bjc.1976.203

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title = "Complement activation in vivo in cancer patients receiving C. Parvum immunotherapy",

abstract = "Serum complement levels were assayed in 26 patients with disseminated cancer, who received immunotherapy with infusion of C. parvum. Complement activation, indicated by the consumption of C3 or C4 or both, was found in 46% of the patients. Serum samples showed direct correlation between decreased C3 and conversion of C3 proactivator, whereas such conversion did not occur when C4 alone was decreased. It is concluded that the bypass (properdin) pathway was activated in patients in whom C3 consumption was detected, while the classical (C1) pathway was activated in the patients with C4 consumption unaccompanied by C3 decrease. Direct correlation was observed between delayed cutaneous hypersensitivity reactions to recall antigens and the incidence of C. parvum-associated complement activation.",

author = "H. Biran and Moake, {J. L.} and Reed, {R. C.} and Gutterman, {J. U.} and Hersh, {E. M.} and Freireich, {E. J.} and Mavligit, {G. M.}",

year = "1976",

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T1 - Complement activation in vivo in cancer patients receiving C. Parvum immunotherapy

AU - Biran, H.

AU - Moake, J. L.

AU - Reed, R. C.

AU - Gutterman, J. U.

AU - Hersh, E. M.

AU - Freireich, E. J.

AU - Mavligit, G. M.

PY - 1976/11

Y1 - 1976/11

N2 - Serum complement levels were assayed in 26 patients with disseminated cancer, who received immunotherapy with infusion of C. parvum. Complement activation, indicated by the consumption of C3 or C4 or both, was found in 46% of the patients. Serum samples showed direct correlation between decreased C3 and conversion of C3 proactivator, whereas such conversion did not occur when C4 alone was decreased. It is concluded that the bypass (properdin) pathway was activated in patients in whom C3 consumption was detected, while the classical (C1) pathway was activated in the patients with C4 consumption unaccompanied by C3 decrease. Direct correlation was observed between delayed cutaneous hypersensitivity reactions to recall antigens and the incidence of C. parvum-associated complement activation.

AB - Serum complement levels were assayed in 26 patients with disseminated cancer, who received immunotherapy with infusion of C. parvum. Complement activation, indicated by the consumption of C3 or C4 or both, was found in 46% of the patients. Serum samples showed direct correlation between decreased C3 and conversion of C3 proactivator, whereas such conversion did not occur when C4 alone was decreased. It is concluded that the bypass (properdin) pathway was activated in patients in whom C3 consumption was detected, while the classical (C1) pathway was activated in the patients with C4 consumption unaccompanied by C3 decrease. Direct correlation was observed between delayed cutaneous hypersensitivity reactions to recall antigens and the incidence of C. parvum-associated complement activation.

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Complement activation in vivo in cancer patients receiving C. Parvum immunotherapy

Abstract

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