Protein kinase A drives paracrine crisis and WNT4-dependent testis tumor in Carney complex
Cyril Djari, … , Antoine Martinez, Anne-Marie Lefrançois-Martinez
Cyril Djari, … , Antoine Martinez, Anne-Marie Lefrançois-Martinez
Published December 1, 2021
Citation Information: J Clin Invest. 2021;131(23):e146910. https://doi.org/10.1172/JCI146910.
View: Text | PDF
Research Article Endocrinology Reproductive biology

Protein kinase A drives paracrine crisis and WNT4-dependent testis tumor in Carney complex

Abstract

Large-cell calcifying Sertoli cell tumors (LCCSCTs) are among the most frequent lesions occurring in male Carney complex (CNC) patients. Although they constitute a key diagnostic criterion for this rare multiple neoplasia syndrome resulting from inactivating mutations of the tumor suppressor PRKAR1A, leading to unrepressed PKA activity, LCCSCT pathogenesis and origin remain elusive. Mouse models targeting Prkar1a inactivation in all somatic populations or separately in each cell type were generated to decipher the molecular and paracrine networks involved in the induction of CNC testis lesions. We demonstrate that the Prkar1a mutation was required in both stromal and Sertoli cells for the occurrence of LCCSCTs. Integrative analyses comparing transcriptomic, immunohistological data and phenotype of mutant mouse combinations led to the understanding of human LCCSCT pathogenesis and demonstrated PKA-induced paracrine molecular circuits in which the aberrant WNT4 signal production is a limiting step in shaping intratubular lesions and tumor expansion both in a mouse model and in human CNC testes.

Authors

Cyril Djari, Isabelle Sahut-Barnola, Amandine Septier, Ingrid Plotton, Nathanaëlle Montanier, Damien Dufour, Adrien Levasseur, James Wilmouth Jr., Jean-Christophe Pointud, Fabio R. Faucz, Crystal Kamilaris, Antoine-Guy Lopez, Florian Guillou, Amanda Swain, Seppo J. Vainio, Igor Tauveron, Pierre Val, Hervé Lefebvre, Constantine A. Stratakis, Antoine Martinez, Anne-Marie Lefrançois-Martinez

×

Figure 4

PKA overactivation alters SC polarity.

Options: View larger image (or click on image) Download as PowerPoint
PKA overactivation alters SC polarity. (A) GSEA enrichment scores of mic...
(A) GSEA enrichment scores of microarray gene expression data using KEGG gene lists associated with junction/cytoskeleton in 2-month-old prKO or srKO testes compared with WT. (B) Heatmap representing the median centered expression of significantly deregulated regulators of cell junctions (for black boxes, adj. P < 0.05) in 2-month-old prKO and srKO testes (n = 3–4) compared with WT (n = 4). (CH) Immunohistochemical detection of β-catenin and CLDN11 and quantification of CLDN11 expression domain based on the distance between basal lamina and apical CLDN11 in 5-week-old WT, prKO, and srKO testes and in normal adult human testis and CNC-LCCSCTs. White lines delineate β-catenin or CLDN11 expression domain. One-way ANOVA was followed by Tukey’s multiple-correction test. (I) Biotin tracer detection after injection underneath the testis capsule in 6-week-old WT, prKO, and srKO testes. White dashed lines mark intraseminiferous biotin diffusion in prKO and srKO testes. (J) BTB integrity loss evaluation based on the percentage of tubule with intraseminiferous biotin accumulation. Scale bars: 100 μm. *P < 0.05; ***P < 0.001.