De Luca, Eliana, Crisi, Paolo Emidio, Marcacci, Maurilia, Malatesta, Daniela, Di Sabatino, Daria, Cito, Francesca, D'Alterio, Nicola, Puglia, Ilaria, Berjaoui, Shadia, Colaianni, Maria Loredana, Tinelli, Antonella, Ripà, Paola, Vincifori, Giacomo, Di Teodoro, Giovanni, Dondi, Francesco, Savini, Giovanni, Boari, Andrea, and Lorusso, Alessio
• Prevalence of FeMV in feline colonies was higher with respect household cats. • FeMVs of this study belong to the genotype 1 and segregate into two clusters. • Isolation has been confirmed to be difficult and time consuming. • No statistically significant correlation was found between FeMV infection and TIN. • Virus histochemistry revealed immunoreactivity in lungs, kidneys and brain sections. Feline morbillivirus (FeMV) is an emerging morbillivirus first described in cats less than a decade ago. FeMV has been associated with chronic kidney disease of cats characterized by tubulointerstitial nephritis (TIN), although this aspect is still controversial and not demonstrated with certainty. To investigate FeMV prevalence and genomic characteristics, an epidemiological survey was conducted in a total number of 127 household cats originating from two Italian regions, Abruzzi and Emilia-Romagna. A total number of 69 cats originating from three feline colonies were also enrolled for the study. Correlation with TIN was investigated by employing a total number of 35 carcasses. Prevalence of FeMV RNA was higher in urine samples collected from cats of colonies (P = 31.8%, CI 95% 22.1–43.6) compared to household cats (P = 8.66%, CI 95% 4.9–14.9) and in young and middle-aged cats while prevalence of FeMV Abs was higher in old cats. Sequences obtained straight from infected biological samples, either partial or complete, cluster into two clades within FeMV genotype 1, distantly related to FeMV genotype 2. Immunohistochemistry analysis of kidney sections of FeMV RNA positive cats revealed immunoreactivity within epithelial cells of renal tubuli and inflammatory cells. However, statistically significant association between FeMV and renal damages, including TIN, was not demonstrated (p= 0.0695, Fisher exact test). By virus histochemistry performed with FeMV-negative feline tissues and a FeMV isolate, tropism for different cellular types such as inflammatory cells residing in blood vessels of kidney and brain, airway epithelial cells, alveolar macrophages and to a lesser extent, the central nervous system, was demonstrated. Additional studies are warranted in order to establish viral tropism and immune response during the early phases of infection and to disentangle the role of FeMV in co-infection processes. [ABSTRACT FROM AUTHOR]