Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts

Maria Krevvata; Barbara C. Silva; John S. Manavalan; Marta Galan-Diez; Aruna Kode; Brya Grace Matthews; David Park; Chiyuan A. Zhang; Naomi Galili; Thomas L. Nickolas; David W. Dempster; William Dougall; Julie Teruya-Feldstein; Aris N. Economides; Ivo Kalajzic; Azra Raza; Ellin Berman; Siddhartha Mukherjee; Govind Bhagat; Stavroula Kousteni

doi:10.1182/blood-2013-07-517219

Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts

Maria Krevvata, Barbara C. Silva, John S. Manavalan, Marta Galan-Diez, Aruna Kode, Brya Grace Matthews, David Park, Chiyuan A. Zhang, Naomi Galili, Thomas L. Nickolas, David W. Dempster, William Dougall, Julie Teruya-Feldstein, Aris N. Economides, Ivo Kalajzic, Azra Raza, Ellin Berman, Siddhartha Mukherjee, Govind Bhagat, Stavroula Kousteni

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

111 Scopus citations

Abstract

The bone marrow niche is thought to act as a permissive microenvironment required for emergence or progression of hematologic cancers. We hypothesized that osteoblasts, components of the niche involved in hematopoietic stem cell (HSC) function, influence the fate of leukemic blasts. We show that osteoblast numbers decrease by 55% in myelodysplasia and acute myeloid leukemia patients. Further, genetic depletion of osteoblasts in mouse models of acute leukemia increased circulating blasts and tumor engraftment in the marrow and spleen leading to higher tumor burden and shorter survival. Myelopoiesis increased and was coupled with a reduction in B lymphopoiesis and compromised erythropoiesis, suggesting that hematopoietic lineage/progression was altered. Treatment of mice with acute myeloid or lymphoblastic leukemia with a pharmacologic inhibitor of the synthesis of duodenal serotonin, a hormone suppressing osteoblast numbers, inhibited loss of osteoblasts. Maintenance of the osteoblast pool restored normal marrow function, reduced tumor burden, and prolonged survival. Leukemia prevention was attributable to maintenance of osteoblast numbers because inhibition of serotonin receptors alone in leukemic blasts did not affect leukemia progression. These results suggest that osteoblasts play a fundamental role in propagating leukemia in the marrow and may be a therapeutic target to induce hostility of the niche to leukemia blasts.

Original language	English
Pages (from-to)	2834-2846
Number of pages	13
Journal	Blood
Volume	124
Issue number	18
DOIs	https://doi.org/10.1182/blood-2013-07-517219
State	Published - 30 Oct 2014
Externally published	Yes

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Krevvata, M., Silva, B. C., Manavalan, J. S., Galan-Diez, M., Kode, A., Matthews, B. G., Park, D., Zhang, C. A., Galili, N., Nickolas, T. L., Dempster, D. W., Dougall, W., Teruya-Feldstein, J., Economides, A. N., Kalajzic, I., Raza, A., Berman, E., Mukherjee, S., Bhagat, G., & Kousteni, S. (2014). Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts. Blood, 124(18), 2834-2846. https://doi.org/10.1182/blood-2013-07-517219

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title = "Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts",

abstract = "The bone marrow niche is thought to act as a permissive microenvironment required for emergence or progression of hematologic cancers. We hypothesized that osteoblasts, components of the niche involved in hematopoietic stem cell (HSC) function, influence the fate of leukemic blasts. We show that osteoblast numbers decrease by 55% in myelodysplasia and acute myeloid leukemia patients. Further, genetic depletion of osteoblasts in mouse models of acute leukemia increased circulating blasts and tumor engraftment in the marrow and spleen leading to higher tumor burden and shorter survival. Myelopoiesis increased and was coupled with a reduction in B lymphopoiesis and compromised erythropoiesis, suggesting that hematopoietic lineage/progression was altered. Treatment of mice with acute myeloid or lymphoblastic leukemia with a pharmacologic inhibitor of the synthesis of duodenal serotonin, a hormone suppressing osteoblast numbers, inhibited loss of osteoblasts. Maintenance of the osteoblast pool restored normal marrow function, reduced tumor burden, and prolonged survival. Leukemia prevention was attributable to maintenance of osteoblast numbers because inhibition of serotonin receptors alone in leukemic blasts did not affect leukemia progression. These results suggest that osteoblasts play a fundamental role in propagating leukemia in the marrow and may be a therapeutic target to induce hostility of the niche to leukemia blasts.",

author = "Maria Krevvata and Silva, {Barbara C.} and Manavalan, {John S.} and Marta Galan-Diez and Aruna Kode and Matthews, {Brya Grace} and David Park and Zhang, {Chiyuan A.} and Naomi Galili and Nickolas, {Thomas L.} and Dempster, {David W.} and William Dougall and Julie Teruya-Feldstein and Economides, {Aris N.} and Ivo Kalajzic and Azra Raza and Ellin Berman and Siddhartha Mukherjee and Govind Bhagat and Stavroula Kousteni",

note = "Publisher Copyright: {\textcopyright} 2014 by The American Society of Hematology.",

year = "2014",

month = oct,

day = "30",

doi = "10.1182/blood-2013-07-517219",

language = "English",

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Krevvata, M, Silva, BC, Manavalan, JS, Galan-Diez, M, Kode, A, Matthews, BG, Park, D, Zhang, CA, Galili, N, Nickolas, TL, Dempster, DW, Dougall, W, Teruya-Feldstein, J, Economides, AN, Kalajzic, I, Raza, A, Berman, E, Mukherjee, S, Bhagat, G & Kousteni, S 2014, 'Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts', Blood, vol. 124, no. 18, pp. 2834-2846. https://doi.org/10.1182/blood-2013-07-517219

TY - JOUR

T1 - Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts

AU - Krevvata, Maria

AU - Silva, Barbara C.

AU - Manavalan, John S.

AU - Galan-Diez, Marta

AU - Kode, Aruna

AU - Matthews, Brya Grace

AU - Park, David

AU - Zhang, Chiyuan A.

AU - Galili, Naomi

AU - Nickolas, Thomas L.

AU - Dempster, David W.

AU - Dougall, William

AU - Teruya-Feldstein, Julie

AU - Economides, Aris N.

AU - Kalajzic, Ivo

AU - Raza, Azra

AU - Berman, Ellin

AU - Mukherjee, Siddhartha

AU - Bhagat, Govind

AU - Kousteni, Stavroula

PY - 2014/10/30

Y1 - 2014/10/30

N2 - The bone marrow niche is thought to act as a permissive microenvironment required for emergence or progression of hematologic cancers. We hypothesized that osteoblasts, components of the niche involved in hematopoietic stem cell (HSC) function, influence the fate of leukemic blasts. We show that osteoblast numbers decrease by 55% in myelodysplasia and acute myeloid leukemia patients. Further, genetic depletion of osteoblasts in mouse models of acute leukemia increased circulating blasts and tumor engraftment in the marrow and spleen leading to higher tumor burden and shorter survival. Myelopoiesis increased and was coupled with a reduction in B lymphopoiesis and compromised erythropoiesis, suggesting that hematopoietic lineage/progression was altered. Treatment of mice with acute myeloid or lymphoblastic leukemia with a pharmacologic inhibitor of the synthesis of duodenal serotonin, a hormone suppressing osteoblast numbers, inhibited loss of osteoblasts. Maintenance of the osteoblast pool restored normal marrow function, reduced tumor burden, and prolonged survival. Leukemia prevention was attributable to maintenance of osteoblast numbers because inhibition of serotonin receptors alone in leukemic blasts did not affect leukemia progression. These results suggest that osteoblasts play a fundamental role in propagating leukemia in the marrow and may be a therapeutic target to induce hostility of the niche to leukemia blasts.

AB - The bone marrow niche is thought to act as a permissive microenvironment required for emergence or progression of hematologic cancers. We hypothesized that osteoblasts, components of the niche involved in hematopoietic stem cell (HSC) function, influence the fate of leukemic blasts. We show that osteoblast numbers decrease by 55% in myelodysplasia and acute myeloid leukemia patients. Further, genetic depletion of osteoblasts in mouse models of acute leukemia increased circulating blasts and tumor engraftment in the marrow and spleen leading to higher tumor burden and shorter survival. Myelopoiesis increased and was coupled with a reduction in B lymphopoiesis and compromised erythropoiesis, suggesting that hematopoietic lineage/progression was altered. Treatment of mice with acute myeloid or lymphoblastic leukemia with a pharmacologic inhibitor of the synthesis of duodenal serotonin, a hormone suppressing osteoblast numbers, inhibited loss of osteoblasts. Maintenance of the osteoblast pool restored normal marrow function, reduced tumor burden, and prolonged survival. Leukemia prevention was attributable to maintenance of osteoblast numbers because inhibition of serotonin receptors alone in leukemic blasts did not affect leukemia progression. These results suggest that osteoblasts play a fundamental role in propagating leukemia in the marrow and may be a therapeutic target to induce hostility of the niche to leukemia blasts.

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U2 - 10.1182/blood-2013-07-517219

DO - 10.1182/blood-2013-07-517219

M3 - Article

C2 - 25139351

AN - SCOPUS:84908587480

SN - 0006-4971

VL - 124

SP - 2834

EP - 2846

JO - Blood

JF - Blood

IS - 18

ER -

Inhibition of leukemia cell engraftment and disease progression in mice by osteoblasts

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