**1. Introduction**

In 1882, when Robert Koch made his ground-breaking announcement that he had discovered, isolated and cultured the bacterium responsible for tuberculosis (TB), there were no curative options for people infected with TB. In Roman times, the personal physician of the emperor Marcus Aurelius (161–180) was prescribing sea trips, fresh air and milk to treat TB patients [1]. English, French and German physicians revisited this concept 17 centuries later. In 1840, the English physician George Bodington wrote an essay "On the treatment and cure of pulmonary consumption," where he recommended fresh, cold and open air, exercise, a healthy diet and wine to treat TB patients. He opposed the treatment popular at the time: confinement of TB patients and the use of drugs such as digitalis and antimony potassium tartrate [2]. The journal Lancet published a harsh review of this essay, describing it as "very crude ideas and unsupported assertions" [3], but later admitted that they had been wrong [4]. Other English physicians followed Bodington's ideas of fresh-air treatment for TB patients but were dismissed by the medical intelligentsia [5]. On the other side of the Channel, the French physician Amédée Latour prescribed sunshine, fresh air, exercise and rich food containing 1/8 oz of sea salt every morning to treat TB [6]. The German physician Hermann Brehmer advocated high altitude, fresh air, exercise and a rich diet with some alcohol for the treatment of TB patients [5]. He opened the first sanatorium in 1854 in Görbersdorf, Prussia, to implement his concept. Sanatoria were beneficial to TB patients with early stages of disease. Lower mortality rates were observed in sanatoria compared to TB patients treated at home [1,7]. Sanatoria would close one hundred years later with the introduction of the first multiantimycobacterial drug regimen to treat TB.

The first drug against the etiologic agent of TB, *Mycobacterium tuberculosis,* was streptomycin, isolated from the soil bacterium *Streptomyces griseus* and shown to have activity against *M. tuberculosis* in 1944 [8,9]. Streptomycin was tested on a 21-year-old woman with advanced pulmonary TB and gave "impressive therapeutic effects" [10,11]. Unfortunately, resistance to streptomycin developed quickly [12,13]. In 1946, Jorgen Lehmann published the discovery of the antimycobacterial activity of para-aminosalicylic acid (PAS) in vitro, in guinea pigs and in TB patients [14]. The addition of PAS to streptomycin treatment drastically reduced the emergence of streptomycin-resistant strains in TB patients but did not abolish it [15]. It would take the introduction of a new TB drug, isoniazid (INH), in 1952 to achieve a successful treatment for TB [16].

INH is one of the most effective drugs against *M. tuberculosis*, which is still used to this day to treat active and latent *M. tuberculosis* infections. INH is part of a four-drug regimen (INH, rifampicin (RIF), ethambutol (EMB) and pyrazinamide (PZA)) to treat drug-susceptible *M. tuberculosis* infection. While RIF targets the RNA polymerase RpoB and PZA's mechanism of action is still unclear, INH and EMB target the mycobacterial cell wall.

The *M. tuberculosis* cell wall has an intricate and unique structure composed of a thick peptidoglycan layer and an outer membrane made up mostly of various lipopolysaccharides and fatty acids with imbedded glycolipids and wax esters. This lipid-rich cell wall forms a low-permeability barrier that protects *M. tuberculosis* against most antibiotics. This is one of the many challenges facing TB drug development and the main reason drug target-based screening has been rather unsuccessful [17,18]. Bacteria require an intact cell membrane in order to survive; therefore, the biosynthesis of cell wall components could be considered a weakness to exploit with new and more potent drugs. The ever-expanding threat of drug resistance should motivate greater alacrity in developing these new therapies. Global drug surveillance data from the World Health Organization indicates that in 2018, half a million people were infected with rifampicin- or multidrug-resistant (MDR) TB, and 6% of them had extensively drug-resistant (XDR) TB [19]. While an MDR *M. tuberculosis* strain is "only" resistant to INH and RIF, an XDR strain is resistant to at least five TB drugs (INH, RIF and three second-line TB drugs). Treatment for drug-resistant TB is very long (minimum 20 months), requiring multiple drugs with potential severe adverse reactions. MDR TB treatment's success rate is approximately 55%, whereas XDR TB is barely 39%. New drugs and shorter drug regimens are actively sought to increase these success rates. This article covers TB drugs specifically targeting the mycobacterial cell wall currently used in clinics or in clinical development, focusing on their discovery, activity, toxicity, mode of action and resistance.
