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“Background Chlamydiae are a large group of obligate intracellular bacteria that includes human pathogens (e.g. Chlamydia trachomatis or C. pneumoniae), animal pathogens (e.g. C. abortus, C. caviae, C. felis, or C. muridarum), or symbionts of free-living

amoebae. Among Chlamydiae, C. trachomatis is a particular clinical and public health concern, being the leading cause of infectious blindness in developing countries [1] and the most prevalent sexually transmitted bacteria worldwide [2]. Like all Chlamydiae, C. trachomatis undergoes a developmental cycle involving the inter-conversion Sclareol between two buy CAL-101 morphologically distinct forms: a non-replicative infectious form, the elementary body (EB), and a replicative non-infectious form, the reticulate body (RB) [3]. Throughout its developmental cycle, C. trachomatis uses a type III secretion system (T3SS) to translocate several effector proteins across the host cell plasma membrane and the inclusion membrane [4, 5]. These T3S effectors are thought to play a central role in bacterial invasion [6, 7] and exit of host cells [8], and in the subversion of various host cell processes [9–16]. There are, however, chlamydial effectors, such as CPAF/CT858 or CT441, which are not T3S substrates [4].