Abstract
In order to sustain a persistent infection, Mycobacterium tuberculosis (Mtb) must adapt to a changing environment that is shaped by the developing immune response. This necessity to adapt is evident in the flexibility of many aspects of Mtb metabolism, including a respiratory chain that consists of two distinct terminal cytochrome oxidase complexes. Under the conditions tested thus far, the bc1/aa3 complex appears to play a dominant role, while the alternative bd oxidase is largely redundant. However, the presence of two terminal oxidases in this obligate pathogen implies that respiratory requirements might change during infection. We report that the cytochrome bd oxidase is specifically required for resisting the adaptive immune response. While the bd oxidase was dispensable for growth in resting macrophages and the establishment of infection in mice, this complex was necessary for optimal fitness after the initiation of adaptive immunity. This requirement was dependent on lymphocyte-derived interferon gamma (IFNγ), but did not involve nitrogen and oxygen radicals that are known to inhibit respiration in other contexts. Instead, we found that ΔcydA mutants were hypersusceptible to the low pH encountered in IFNγ-activated macrophages. Unlike wild type Mtb, cytochrome bd-deficient bacteria were unable to sustain a maximal oxygen consumption rate (OCR) at low pH, indicating that the remaining cytochrome bc1/aa3 complex is preferentially inhibited under acidic conditions. Consistent with this model, the potency of the cytochrome bc1/aa3 inhibitor, Q203, is dramatically enhanced at low pH. This work identifies a critical interaction between host immunity and pathogen respiration that influences both the progression of the infection and the efficacy of potential new TB drugs.
Highlights
Tuberculosis (TB) is responsible for an estimated 1.4 million deaths annually and remains one of the most deadly infectious diseases [1]
The mycobacterial electron transport chain (ETC) has two terminal oxidases, the cytochrome bc1/aa3 super complex that is related to mitochondrial complex III and IV, and the cytochrome bd oxidase which is unique to prokaryotes
The latter complex in Mycobacterium tuberculosis (Mtb) is encoded in a single operon, cydABDC, which produces both the cydAB oxidase complex and cydDC, a putative ABC-transporter that has not been studied in Mtb, but is necessary for assembly of the cytochrome in Escherichia coli [8,9]
Summary
Tuberculosis (TB) is responsible for an estimated 1.4 million deaths annually and remains one of the most deadly infectious diseases [1]. The mycobacterial ETC has two terminal oxidases, the cytochrome bc1/aa super complex that is related to mitochondrial complex III and IV, and the cytochrome bd oxidase which is unique to prokaryotes These terminal oxidases transfer electrons from the ETC to O2 and contribute to the proton motive force (PMF) gradient that powers the production of ATP by ATP synthase. Both genetic [2] and chemical inhibition of the cytochrome bc1/aa3 [3,4,5] has been used to show that this complex is required for optimal growth and persistence during infection, and cytochrome bc1/aa inhibitors are under evaluation as antimycobacterial therapies [6]. While it is clear that the cytochrome bd oxidase is active in mycobacteria, the non-redundant role of this system during infection is unknown
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