Antibody News

By Jacqueline Carrico, BS, MD Candidate

Chimeric antigen receptor T-cells, better known as CAR-T cells, are being used as a novel anticancer therapy. CAR-T cells are engineered T-cells which express a modified antigen-receptor. Each chimeric antigen receptor contains 3 domains: an extracellular binding domain, a transmembrane hinge domain, and an intracellular activation or costimulatory domain. The extracellular portion is the single chain variable fragment (scFv), made up of an antibody-derived heavy chain and light chain, which ultimately recognize specific tumor antigens. The intracellular activation domain allows T-cell activation upon...

By Jamshed Arslan Pharm.D.

von Hippel-Lindau (VHL) disease is associated with tumors arising in multiple organs. Activation of hypoxia-inducible factor (HIF)-alpha underlies the VHL disease pathogenesis. In normoxia, VHL tumor-suppressor protein (pVHL) and E3 ubiquitin ligase lead to proteosomal degradation of HIF-alpha. In hypoxia, HIF-alpha escapes degradation, partly because pVHL binding to HIF-alpha depends on a posttranslational modification (hydroxylation of proline residues) on HIF-alpha that only occurs in normoxia. The exact role of pVHL in tumor hypoxia, when HIF-alpha is stabilized, is poorly...

By Jamshed Arslan Pharm.D.

Neuromuscular disorders affect the peripheral nervous system and muscles. Spinal muscular atrophy (SMA) is one such incurable disease in which muscles fail to receive signals from the spinal motor neurons (MNs), and consequently, weaken due to inactivity. MN degeneration and muscle atrophy lead to the premature death of the victims. Like most of the neuromuscular disorders, SMA is genetic, and its genetic causes are known: the inactivation of survival motor neuron 1 (SMN1) gene, which reduces the...

By Christina Towers, PhD.

Misfolded and damaged proteins are degraded by two canonical mechanisms in the cell including the ubiquitin-mediated proteasome system (UPS) and autophagy.  Proteins can be targeted for degradation by their N-terminal amino acid which can be modified to become an N-degron.  N-degrons allow for selective degradation first through the UPS, however, if the proteasome is not highly functional, these proteins may be degraded via autophagy, a lysosomal mediated form of proteolysis ¹. While many studies have shown that...

By Jamshed Arslan Pharm.D.

Multiple myeloma (MM) is a cancer of antibody-producing plasma cells. The bone marrow (BM) of MM patients is hypoxic, and MM cells overexpress many cancerous genes that are regulated by hypoxia-inducible factors (HIFs). Cancer stem cells (CSCs) in the hypoxic BM regions are blamed for the incurability of MM, because CSCs are often resistant to drugs currently used against BM cancers (including proteasome inhibitors and immunomodulatory agents). Dr. Eishi Ashihara at the Kyoto Pharmaceutical University, Japan, and colleagues, set out to characterize the biology of MM stem cells. They found that TGF-beta...

Therapeutic proteins such as monoclonal antibodies (mAbs) can be subject to physical or chemical stress during the manufacturing process and supply chain. A common chemical degradation is the deamidation of the amino acid asparagine to aspartic acid or iso-aspartic acid. Modification of glutamine to glutamic acid is also possible, although this occurs at a slower rate. When deamidation occurs in the antigen binding region of the mAb, it can result in a loss of potency. This sequence liability may be defined as a critical quality attribute and represents a risk to the development of novel biologics and biosimilars alike.  As such, it is important to have reliable protein characterization methods with sufficient sensitivity and selectivity to identify and quantify levels of deamidation.

Physicochemical analysis

The transformation of an amide side-chain, via a succinimide intermediate, to a carboxylic acid results in a change in the net charge of the...

By Jamshed Arslan Pharm.D.

Interneurons transmit impulses between other neurons, in part, to facilitate the birth of neurons. Cortical interneurons themselves arise from the progenitors in the ventral telencephalon, a brain region that generates basal ganglia. The role of mechanistic target of rapamycin (MTOR) signaling in this process is poorly understood, even though MTOR is known to determine brain size. By deleting Mtor in mouse interneuron progenitors and their progeny, Dr. Woo-Yang Kim’s team at the University of Nebraska Medical Center, USA, found two homeostatic activities of MTOR in the developing brain: regulation of autophagy and...

By Yoskaly Lazo-Fernandez, PhD

The first description of what is called today an autophagosome was given in a paper published in 1957. Its author employed electron microscopy to observe the neonatal features of mouse kidneys¹. Autophagosomes where then described as large round bodies found in the cytoplasm, primarily of proximal tubule epithelial cells, and consisting of an amorphous material containing concentrically lamellar structures and mitochondria. It was not by chance that these structures were found in kidney tubules, because autophagy plays an essential role in kidney function both in health and disease^2,3. This blog will briefly introduce the main...

By Jamshed Arslan Pharm.D.

Muscle atrophy is a common feature of many tumors. Cancer-induced muscle wasting, or cancer cachexia, results from pro-inflammatory cytokines (TNFα and IL-6) and/or agonists of type IIB activin receptors (ActRIIB), but the key humoral factors have remained elusive. Animal studies have implicated systemic inflammation-induced activation of p38β MAPK-C/EBPβ signaling, but the etiology of cancer cachexia was unclear until recently. A team led by researchers at the University of...

By Yoskaly Lazo-Fernandez, PhD

The cell surface receptor CD95 (also known as Fas or APO-1) is the best-characterized member of the tumor necrosis factor (TNF) receptor superfamily¹. Many receptors in this family, including CD95 are called Death Receptors because of their ability to induce apoptosis². In cells expressing CD95, apoptosis is triggered by the binding of this receptor’s specific ligand, CD95L. This mechanism, which was originally discovered in the early nineties, allows CD95L...

By Christina Towers, PhD.

It has long been known that programmed cell death can take place in many forms.  The most well characterized form, apoptosis, occurs when either extrinsic or intrinsic stimuli stimulate signaling cascades that result in a series of caspase cleavage events resulting in cleavage and activation of the effector caspase-3.  The end result is cell shrinkage, condensation and cleavage of chromosomal DNA, and plasma membrane blebbing that leaves the cell membrane intact¹.  Apoptotic cells are engulfed by antigen presenting cells and induce anti-inflammatory and tolerogenic immune responses².  Alternatively, necroptosis, a programmed form of necrosis, is less characterized.  However, it is now known that this process is also tightly regulated and mediated by a complex...