Author
Listed:
- Ruda de Luna Almeida Santos
(Van Andel Research Institute)
- Lin Bai
(Van Andel Research Institute)
- Pradeep K. Singh
(Weill Cornell Medicine)
- Naoka Murakami
(Renal Division, Brigham and Women’s Hospital, Harvard Medical School)
- Hao Fan
(Weill Cornell Medicine)
- Wenhu Zhan
(Weill Cornell Medicine)
- Yingrong Zhu
(Weill Cornell Medicine)
- Xiuju Jiang
(Weill Cornell Medicine)
- Kaiming Zhang
(Baylor College of Medicine)
- Jean Pierre Assker
(Renal Division, Brigham and Women’s Hospital, Harvard Medical School)
- Carl F. Nathan
(Weill Cornell Medicine)
- Huilin Li
(Van Andel Research Institute)
- Jamil Azzi
(Renal Division, Brigham and Women’s Hospital, Harvard Medical School)
- Gang Lin
(Weill Cornell Medicine)
Abstract
Proteasome inhibitors benefit patients with multiple myeloma and B cell-dependent autoimmune disorders but exert toxicity from inhibition of proteasomes in other cells. Toxicity should be minimized by reversible inhibition of the immunoproteasome β5i subunit while sparing the constitutive β5c subunit. Here we report β5i-selective inhibition by asparagine-ethylenediamine (AsnEDA)-based compounds and present the high-resolution cryo-EM structural analysis of the human immunoproteasome. Despite inhibiting noncompetitively, an AsnEDA inhibitor binds the active site. Hydrophobic interactions are accompanied by hydrogen bonding with β5i and β6 subunits. The inhibitors are far more cytotoxic for myeloma and lymphoma cell lines than for hepatocarcinoma or non-activated lymphocytes. They block human B-cell proliferation and promote apoptotic cell death selectively in antibody-secreting B cells, and to a lesser extent in activated human T cells. Reversible, β5i-selective inhibitors may be useful for treatment of diseases involving activated or neoplastic B cells or activated T cells.
Suggested Citation
Ruda de Luna Almeida Santos & Lin Bai & Pradeep K. Singh & Naoka Murakami & Hao Fan & Wenhu Zhan & Yingrong Zhu & Xiuju Jiang & Kaiming Zhang & Jean Pierre Assker & Carl F. Nathan & Huilin Li & Jamil , 2017.
"Structure of human immunoproteasome with a reversible and noncompetitive inhibitor that selectively inhibits activated lymphocytes,"
Nature Communications, Nature, vol. 8(1), pages 1-11, December.
Handle:
RePEc:nat:natcom:v:8:y:2017:i:1:d:10.1038_s41467-017-01760-5
DOI: 10.1038/s41467-017-01760-5
Download full text from publisher
Corrections
All material on this site has been provided by the respective publishers and authors. You can help correct errors and omissions. When requesting a correction, please mention this item's handle: RePEc:nat:natcom:v:8:y:2017:i:1:d:10.1038_s41467-017-01760-5. See general information about how to correct material in RePEc.
If you have authored this item and are not yet registered with RePEc, we encourage you to do it here. This allows to link your profile to this item. It also allows you to accept potential citations to this item that we are uncertain about.
We have no bibliographic references for this item. You can help adding them by using this form .
If you know of missing items citing this one, you can help us creating those links by adding the relevant references in the same way as above, for each refering item. If you are a registered author of this item, you may also want to check the "citations" tab in your RePEc Author Service profile, as there may be some citations waiting for confirmation.
For technical questions regarding this item, or to correct its authors, title, abstract, bibliographic or download information, contact: Sonal Shukla or Springer Nature Abstracting and Indexing (email available below). General contact details of provider: http://www.nature.com .
Please note that corrections may take a couple of weeks to filter through
the various RePEc services.
Printed from https://ideas.repec.org/a/nat/natcom/v8y2017i1d10.1038_s41467-017-01760-5.html
My bibliography
Save this article