Synthesis and In Vitro Applications of Ice Recrystallization Inhibitors
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Université d'Ottawa / University of Ottawa
Abstract
Abstract
Recent advances in the clinical diagnosis and treatment of diseases using cell
transplantation have emphasized the urgent need to cryopreserve many types of cells. In
transfusion medicine, red blood cell (RBC) transfusions are used to treat anemia and
inherited blood disorders, replace blood lost during or after surgery and treat accident
victims and mass casualty events. In regenerative medicine, mesenchymal stem cell
(MSC) therapy offers promising treatment for tissue injury and immune disorders.
Current cryoprotective agents (CPAs) utilized for RBCs and MSCs are 40% glycerol and
10% dimethyl sulfoxide (DMSO), respectively. Although glycerol is required for
successful cryopreservation of RBCs, it must be removed from RBCs post-thaw using
costly and time-consuming deglycerolization procedures to avoid intravascular
hemolysis. Unfortunately, while DMSO prevents cell damage and increases post-thaw
MSC viability and recovery, recent reports have suggested that MSCs cryopreserved in
DMSO display compromised function post-thaw. As a result, improvements to the
current cryopreservation protocols such as reducing post-thaw RBC processing times and
improving MSC function post-thaw are necessary in order to meet the increasing
demands of emerging cellular therapies.
Ice recrystallization has been identified as a significant contributor to cellular injury
and death during cryopreservation. Consequently, the ability to inhibit ice
recrystallization is a very desirable property for an effective CPA, unlike the
conventional CPAs such as DMSO and glycerol that function via a different mechanism
and do not control or inhibit ice recrystallization. Over the past few years, our laboratory
has reported several different classes of small molecules capable of inhibiting ice
recrystallization such as lysine-based surfactants, non-ionic carbohydrate-based
amphiphiles (alkyl and aryl aldonamides) and O-linked alkyl and aryl glycosides. The use
of these small molecule ice recrystallization inhibitors (IRIs) as novel CPAs has become
an important strategy to improve cell viability and function post-thaw.
With the overall goal to identify highly effective inhibitors of ice recrystallization, the
first part of this thesis examines the IRI activity of three diverse classes of small
molecules including carbohydrate-based surfactants bearing an azobenzene moiety,
fluorinated aryl glycosides and phosphate sugars. While the majority of the carbohydrate-
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Keywords
Cryopreservation, Ice Recrystallization Inhibition, Red Blood Cells, Mesenchymal Stem Cells, Cryoprotectants
