HilE mediates motility thermoregulation in typhoidal Salmonella serovars at elevated physiological temperatures

Salmonella enterica is a diverse bacterial pathogen consisting of both typhoidal and nontyphoidal clinically distinct serovars. While typhoidal serovars cause in humans a systemic life-threatening enteric fever, nontyphoidal Salmonella (NTS) usually provoke a localized self-limiting gastroenteritis. Factors responsible for the different diseases caused by distinct Salmonella serovars are still poorly understood. Here, we show that at elevated physiological temperature, manifested during enteric fever (39-40°C), the transcription of the flagellar regulon, its protein translation, and flagella-mediated motility are all repressed in the typhoidal serovar, S . Paratyphi A (SPA). In contrast, the NTS representative serovar, S . Typhimurium, maintains similar or even higher levels of flagellar genes transcription, translation, and motility at 40°C relative to 37°C. By using a temperature-responsive flagellar reporter system in conjunction with a dense transposon mutagenesis screen we found that under elevated temperature, HilE negatively regulates SPA motility in a HilD-dependent manner. Since HilD is required for the transcriptional activation of FlhDC, the master regulator of the Salmonella flagellar-chemotaxis regulon, null deletion of hilE leads to motility upregulation at elevated temperature and the loss of motility thermoregulation in SPA. Interestingly, the absence of HilE also leads to a hyper-uptake of SPA by THP- 1 human macrophages at 40°C, but not at 37°C. Moreover, we show that a HilE-mediated motility thermoregulation is common to other typhoidal serovars, including S . Typhi and S . Sendai, but not to S . Paratyphi B, nor to various NTS serovars. Based on these results, we propose that HilE plays a unique role in motility thermoregulation in typhoidal Salmonella in a way that may restrain systemic dissemination of the pathogen via professional phagocytes, during the acute phase of enteric fever.