The role of the CD28-CD86 signaling module in maintaining myeloma cell viability Público

Abstract

Multiple myeloma is an incurable hematologic malignancy of long-lived antibody secreting cells. Despite advances in therapeutics in the past decade that have led to vastly improved patient outcomes, there is still no known cure. Myeloma cells resemble their normal counterpart, long-lived plasma cells that reside in the bone marrow, to such an extent that survival factors that regulate plasma cell survival have also been shown to be required to maintain myeloma cell viability. A reliance on the bone marrow microenvironment for growth and survival signals is a characteristic shared by normal and malignant plasma cells. These signals are mediated by interactions between the myeloma cells and other components of the bone marrow stroma. We hypothesize that disrupting these interactions can induce apoptosis in myeloma cells, providing another means to target this disease.

We propose that one interaction that could be targeted for clinical benefit in myeloma is that between CD28 and CD86. These molecules are better characterized for their role in T-cell costimulation, however the signaling pathway/s they mediate have been shown to be important in maintaining plasma cell longevity in murine models. Previous studies from our lab have shown that activation of the CD28 pathway can protect myeloma cells against different death signals. These molecules are frequently expressed in myeloma cells, thus research into the signals relayed by this module is important to determine the role/s it plays in myeloma pathogenesis.

Our data shows that blockade of this pathway by inhibiting expression of either CD28 or CD86 with shRNAs leads to myeloma cell death. When we investigated gene expression changes when either molecule was silenced, we found that one of the genes that was down-regulated with CD28 or CD86 silencing was IRF4, a well-known myeloma survival factor. We also found that modulation of this signaling pathway led to downregulation in the expression of integrins, and solute carrier (SLC) family members, showing that this pathway regulates multiple aspects of myeloma physiology that are important in maintaining viability and function.

Interestingly, our data also shows that CD86, the canonical ligand in this signaling module, has signaling capacity. Overexpression of full-length CD86 protects myeloma cells against different death signals. In contrast, a “tail-less” version of CD86 could not protect against the same insults, indicating that CD86 is relaying a pro-survival signal in myeloma cells that is dependent on its cytoplasmic tail. Altogether, our data indicates that further investigation of the signals mediated by the CD28-CD86 signaling module is warranted in the context of myeloma, given that these two molecules are regulating important myeloma survival factors.

Table of Contents

I. Introduction. 1

A. Myeloma cells are long-lived bone marrow plasma cells gone awry. 2

Myeloma cells retain plasma cell function and longevity. 2

Myeloma cells, like most long-lived plasma cells, arise from the germinal center reaction. 5

Plasma cell programming is maintained in myeloma cells. 8

Plasma cells rely on protein processing pathways, as do myeloma cells. 11

B. Survival signaling requirements for bone marrow plasma cells are also necessary for myeloma cells. 13

MCL-1 is required for both normal and malignant plasma cell survival 14

Receptor-Ligand interactions play important roles in plasma cell survival 15

C. CD28-CD86 signaling regulates a prosurvival signal in normal and malignant plasma cells. 19

CD28 mediates immune activation in T cells. 19

CD28 in normal plasma cells. 21

CD28 and its role in malignant plasma cells. 22

CD86 is a CD28 ligand and has a distinct function from CD80. 24

CD86 and what is known about its downstream signaling effectors. 25

CD86 in B cell differentiation. 27

CD86 in hematologic malignancies. 27

Blockade of CD28-CD86 as a therapeutic avenue for myeloma. 27

II. CD86 regulates myeloma cell survival 29

Abstract. 29

Introduction. 29

Materials and Methods. 30

Results. 33

CD28 and CD86 expression influence patient outcomes. 33

Blockade of CD86 expression leads to myeloma cell death. 35

Gene expression changes in CD28 versus CD86-silenced cells are consistent with regulation of both distinct and common pathways, including expression of IRF4. 36

The cytoplasmic tail of CD86 plays a role in CD28-CD86 function. 38

Overexpression of shRNA-resistant full length CD86 protects against CD28- and CD86- silencing, but not against loss of IRF4. 39

Overexpression of pro-survival Bcl-2 family members leads to partial inhibition of CD86-knockdown induced death. 40

Discussion. 42

Figure Legends. 48

Supplementary Methods and Data. 59

Table S1. List of Cell lines and sources. 61

Table S2. List of shRNA clones used in this study. 61

Table S3. List of antibodies used for flow cytometry and Western Blotting. 62

Table S4. List of qRT-PCR probes used for measuring mRNA expression levels. 63

III. The CD28-CD86 signaling pathway plays a role in the regulation of SLC7A5. 73

Introduction. 73

Results. 73

Silencing of CD28 or CD86 results in downregulation of SLC7A5. 73

Overexpression of CD86 results in modest protection against cell death induced by silencing of SLC7A5. 74

Discussion. 74

Figures. 77

IV. CTLA-4-Ig and it’s potential for therapeutic use in myeloma. 79

Introduction. 79

Materials and Methods. 81

Results. 83

CTLA-4-Ig induces cell death in myeloma cells in vitro. 83

Treatment with CTLA-4-Ig leads to downregulation of many of the same genes as silencing of CD28 or CD86. 83

Cell death induced by physical blockade of CD28-CD86 interaction is both caspase -dependent and -independent. 84

Overexpression of CD86FLm could not protect against cell death induced by CTLA-4-Ig. 84

Discussion. 85

Figures. 87

V. Discussion. 91

CD28 and CD86 are commonly expressed on myeloma cells from primary cells. 91

Blockade of CD28-CD86 signaling in primary myeloma cells results in cell death. 93

CD28-CD86 signaling regulates different factors involved in myeloma cell survival 94

CD86 has signaling capacity. 99

Comparing silencing of CD28 or CD86 with blockade using CTLA-4-Ig. 102

Manipulation of the CD28-CD86 pathway as a therapeutic avenue in myeloma. 104

Future directions. 107

Literature Cited. 110

About this Dissertation

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School	Laney Graduate School
Department	Biological and Biomedical Sciences
Subfield / Discipline	Immunology and Molecular Pathogenesis
Degree	Ph.D.
Submission	Dissertation
Language	English
Research Field	Biology, Cell Biology, Molecular
Palavra-chave	Cancer Biology Immunology Myeloma
Committee Chair / Thesis Advisor	Boise, Lawrence H., Emory University
Committee Members	Jacob, Joshy, Emory University Evavold, Brian D., University of Utah Boss, Jeremy M., Emory University Chen, Jing, Emory University

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