Selective apoptotic killing of malignant hemopoietic cells by antibody-targeted delivery of an amphipathic peptide

Alexandra J. Marks; Margaret S. Cooper; Robert J. Anderson; Kim H. Orchard; Geoffrey Hale; Janet M. North; Kanagasabai Ganeshaguru; Andrew J. Steele; Atul B. Mehta; Mark W. Lowdell; R. Gitendra Wickremasinghe

doi:10.1158/0008-5472.CAN-04-2594

Selective apoptotic killing of malignant hemopoietic cells by antibody-targeted delivery of an amphipathic peptide

Alexandra J. Marks, Margaret S. Cooper, Robert J. Anderson, Kim H. Orchard, Geoffrey Hale, Janet M. North, Kanagasabai Ganeshaguru, Andrew J. Steele, Atul B. Mehta, Mark W. Lowdell, R. Gitendra Wickremasinghe

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

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Abstract

The α-helical amphipathic peptide D-(KLAKLAK)₂ is toxic to enkaryotic cells if internalized by a suitable targeting mechanism. We have targeted this peptide to malignant hemopoietic cells via conjugation to monoclonal antibodies, which recognize lineage-specific cell surface molecules. An anti-CD19/peptide conjugate efficiently killed 3/3 B lymphoid lines. However, an anti-CD33/peptide conjugate was cytotoxic to only one of three CD33-positive myeloid leukemia lines. The IC₅₀ towards susceptible lines were in the low nanomolar range. Conjugates were highly selective and did not kill cells that did not express the appropriate cell surface cognate of the antibody moiety. Anti-CD19/peptide conjugates efficiently killed cells from patients with chronic lymphocytic leukemia but anti-CD33/peptide reagents were less effective against fresh acute myeloid leukemia cells. We therefore suggest that amphipathic peptides may be of value as targeted therapeutic agents for the treatment of a subset of hematologic malignancies.

Original language	English
Pages (from-to)	2373-2377
Number of pages	5
Journal	Cancer Research
Volume	65
Issue number	6
DOIs	https://doi.org/10.1158/0008-5472.CAN-04-2594
Publication status	Published - Mar 15 2005
Externally published	Yes

ASJC Scopus Subject Areas

Oncology
Cancer Research

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1158/0008-5472.CAN-04-2594

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Marks, A. J., Cooper, M. S., Anderson, R. J., Orchard, K. H., Hale, G., North, J. M., Ganeshaguru, K., Steele, A. J., Mehta, A. B., Lowdell, M. W., & Wickremasinghe, R. G. (2005). Selective apoptotic killing of malignant hemopoietic cells by antibody-targeted delivery of an amphipathic peptide. Cancer Research, 65(6), 2373-2377. https://doi.org/10.1158/0008-5472.CAN-04-2594

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title = "Selective apoptotic killing of malignant hemopoietic cells by antibody-targeted delivery of an amphipathic peptide",

abstract = "The α-helical amphipathic peptide D-(KLAKLAK)2 is toxic to enkaryotic cells if internalized by a suitable targeting mechanism. We have targeted this peptide to malignant hemopoietic cells via conjugation to monoclonal antibodies, which recognize lineage-specific cell surface molecules. An anti-CD19/peptide conjugate efficiently killed 3/3 B lymphoid lines. However, an anti-CD33/peptide conjugate was cytotoxic to only one of three CD33-positive myeloid leukemia lines. The IC50 towards susceptible lines were in the low nanomolar range. Conjugates were highly selective and did not kill cells that did not express the appropriate cell surface cognate of the antibody moiety. Anti-CD19/peptide conjugates efficiently killed cells from patients with chronic lymphocytic leukemia but anti-CD33/peptide reagents were less effective against fresh acute myeloid leukemia cells. We therefore suggest that amphipathic peptides may be of value as targeted therapeutic agents for the treatment of a subset of hematologic malignancies.",

author = "Marks, {Alexandra J.} and Cooper, {Margaret S.} and Anderson, {Robert J.} and Orchard, {Kim H.} and Geoffrey Hale and North, {Janet M.} and Kanagasabai Ganeshaguru and Steele, {Andrew J.} and Mehta, {Atul B.} and Lowdell, {Mark W.} and Wickremasinghe, {R. Gitendra}",

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doi = "10.1158/0008-5472.CAN-04-2594",

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AU - Marks, Alexandra J.

AU - Cooper, Margaret S.

AU - Anderson, Robert J.

AU - Orchard, Kim H.

AU - Hale, Geoffrey

AU - North, Janet M.

AU - Ganeshaguru, Kanagasabai

AU - Steele, Andrew J.

AU - Mehta, Atul B.

AU - Lowdell, Mark W.

AU - Wickremasinghe, R. Gitendra

PY - 2005/3/15

Y1 - 2005/3/15

N2 - The α-helical amphipathic peptide D-(KLAKLAK)2 is toxic to enkaryotic cells if internalized by a suitable targeting mechanism. We have targeted this peptide to malignant hemopoietic cells via conjugation to monoclonal antibodies, which recognize lineage-specific cell surface molecules. An anti-CD19/peptide conjugate efficiently killed 3/3 B lymphoid lines. However, an anti-CD33/peptide conjugate was cytotoxic to only one of three CD33-positive myeloid leukemia lines. The IC50 towards susceptible lines were in the low nanomolar range. Conjugates were highly selective and did not kill cells that did not express the appropriate cell surface cognate of the antibody moiety. Anti-CD19/peptide conjugates efficiently killed cells from patients with chronic lymphocytic leukemia but anti-CD33/peptide reagents were less effective against fresh acute myeloid leukemia cells. We therefore suggest that amphipathic peptides may be of value as targeted therapeutic agents for the treatment of a subset of hematologic malignancies.

AB - The α-helical amphipathic peptide D-(KLAKLAK)2 is toxic to enkaryotic cells if internalized by a suitable targeting mechanism. We have targeted this peptide to malignant hemopoietic cells via conjugation to monoclonal antibodies, which recognize lineage-specific cell surface molecules. An anti-CD19/peptide conjugate efficiently killed 3/3 B lymphoid lines. However, an anti-CD33/peptide conjugate was cytotoxic to only one of three CD33-positive myeloid leukemia lines. The IC50 towards susceptible lines were in the low nanomolar range. Conjugates were highly selective and did not kill cells that did not express the appropriate cell surface cognate of the antibody moiety. Anti-CD19/peptide conjugates efficiently killed cells from patients with chronic lymphocytic leukemia but anti-CD33/peptide reagents were less effective against fresh acute myeloid leukemia cells. We therefore suggest that amphipathic peptides may be of value as targeted therapeutic agents for the treatment of a subset of hematologic malignancies.

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Selective apoptotic killing of malignant hemopoietic cells by antibody-targeted delivery of an amphipathic peptide

Abstract

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UN SDGs

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