18 research outputs found
Insights into Current Tropomyosin Receptor Kinase (TRK) inhibitors: development and clinical application
The use of kinase-directed precision medicine has been heavily pursued since the discovery and development of
imatinib. Annually, it is estimated that around ā¼20 000 new cases of tropomyosin receptor kinase (TRK) cancers are diagnosed,
with the majority of cases exhibiting a TRK genomic rearrangement. In this Perspective, we discuss current development and
clinical applications for TRK precision medicine by providing the following: (1) the biological background and significance of
the TRK kinase family, (2) a compilation of known TRK inhibitors and analysis of their cocrystal structures, (3) an overview of
TRK clinical trials, and (4) future perspectives for drug discovery and development of TRK inhibitors
Differentiation induced by physiological and pharmacological stimuli leads to increased antigenicity of human neuroblastoma cells
Sympathetic neuronal differentiation is associated with favorable prognosis of neuroblastoma (NB), the most common extra-cranial solid tumor of early childhood. Differentiation agents have proved useful in clinical protocols of NB treatment, but using them as a sole treatment is not sufficient to induce tumor elimination in patients. Therefore, complementary approaches, such as immunotherapy, are warranted. Here we demonstrate that differentiation of NB cell lines and ex vivo isolated tumor cells in response to physiological or pharmacological stimuli is associated with acquisition of increased antigenicity. This manifests as increased expression of surface major histocompatibility class I complexes and ICAM-1 molecules and translates into increased sensitivity of NB cells to lysis by cytotoxic T lymphocytes (CTLs) and natural killer (NK) cells. The latter is paralleled by enhanced ability of differentiated cells to form immune conjugates and bind increased amounts of granzyme B to the cell surface. We demonstrate, for the first time, that, regardless of the stimulus applied, the differentiation state in NBs is associated with increased tumor antigenicity that enables more efficient elimination of tumor cells by cytotoxic lymphocytes and paves the way for combined application of differentiation-inducing agents and immunotherapy as an auxiliary approach in NB patients
Protein Kinase CĪµ Actin-binding Site Is Important for Neurite Outgrowth during Neuronal Differentiation
We have previously shown that protein kinase CĪµ (PKCĪµ) induces neurite outgrowth via its regulatory domain and independently of its kinase activity. This study aimed at identifying mechanisms regulating PKCĪµ-mediated neurite induction. We show an increased association of PKCĪµ to the cytoskeleton during neuronal differentiation. Furthermore, neurite induction by overexpression of full-length PKCĪµ is suppressed if serum is removed from the cultures or if an actin-binding site is deleted from the protein. A peptide corresponding to the PKCĪµ actin-binding site suppresses neurite outgrowth during neuronal differentiation and outgrowth elicited by PKCĪµ overexpression. Neither serum removal, deletion of the actin-binding site, nor introduction of the peptide affects neurite induction by the isolated regulatory domain. Membrane targeting by myristoylation renders full-length PKCĪµ independent of both serum and the actin-binding site, and PKCĪµ colocalized with F-actin at the cortical cytoskeleton during neurite outgrowth. These results demonstrate that the actin-binding site is of importance for signals acting on PKCĪµ in a pathway leading to neurite outgrowth. Localization of PKCĪµ to the plasma membrane and/or the cortical cytoskeleton is conceivably important for its effect on neurite outgrowth