Discovery of Orally Active Hydroxyethylamine Based SPPL2a Inhibitors.

Authors :: Velcicky J
Mathison CJN
Nikulin V
Pflieger D
Epple R
Azimioara M
Cow C
Michellys PY
Rigollier P
Beisner DR
Bodendorf U
Guerini D
Liu B
Wen B
Zaharevitz S
Brandl T
Source :: ACS medicinal chemistry letters [ACS Med Chem Lett] 2019 May 23; Vol. 10 (6), pp. 887-892. Date of Electronic Publication: 2019 May 23 (Print Publication: 2019).
Publication Year :: 2019
Abstract: SPPL2a (Signal Peptide Peptidase Like 2a) is an intramembrane aspartyl protease engaged in the function of B-cells and dendritic cells. Despite being an attractive target for modulation of the immune system, selective SPPL2a inhibitors are barely described in the literature. Recently, we have disclosed a selective, small molecular weight agent SPL-707 which confirmed that pharmacological inhibition of SPPL2a leads to the accumulation of its substrate CD74/p8 and as a consequence to a reduction in the number of B-cells as well as myeloid dendritic cells in mice. In this paper we describe the discovery of novel hydroxyethylamine based SPPL2a inhibitors. Starting from a rather lipophilic screening hit, several iterative optimization cycles allowed for its transformation into a highly potent and selective compound 15 ( SPL-410 ) which inhibited in vivo CD74/p8 fragment processing in mice at 10 mg/kg oral dose.<br />Competing Interests: The authors declare no competing financial interest.