key: cord-1011135-4x9anilx
authors: Meini, Simone; Pagotto, Alberto; Longo, Benedetta; Vendramin, Igor; Pecori, Davide; Tascini, Carlo
title: Role of Lopinavir/Ritonavir in the Treatment of Covid-19: A Review of Current Evidence, Guideline Recommendations, and Perspectives
date: 2020-06-30
journal: J Clin Med
DOI: 10.3390/jcm9072050
sha: ab10efadcbf12ffea4252cf2dd644bf017e70fd2
doc_id: 1011135
cord_uid: 4x9anilx

A life-threatening respiratory illness (COVID-19) due to severe acute respiratory syndrome (SARS)-CoV-2 coronavirus was first described in December 2019 in Wuhan (China), rapidly evolving into a pandemic. In the first phase, when the viral replication plays a pivotal pathogenetic role, antiviral drugs could be crucial in limiting viral-induced organ damage. Unfortunately, there are no specific antivirals of proven efficacy for COVID-19, and several drugs have been repurposed to face this dramatic pandemic. In this paper we review the studies evaluating lopinavir/ritonavir association (LPV/r) use in COVID-19, and previously in SARS and Middle East respiratory syndrome (MERS). We searched PubMed to identify all relevant clinical and laboratory studies published up to 15 May 2020; the guidelines on the use of LPV/r in COVID-19 were further directly searched on the website of the main international scientific societies and agencies. Available evidence is currently scarce and of low quality. The recommendations issued for COVID-19 vary from positions clearly against the use of LPV/r to other positions that are more favorable. In our opinion, despite the controversial results of an important randomized clinical trial, and some recommendations, clinicians should not abandon the use of LPV/r for the treatment of COVID-19, possibly using this drug inside a prospective randomized trial, waiting for the results of the numerous ongoing trials evaluating its efficacy.

Starting in December 2019 in Wuhan (Hubei province, China), a novel coronavirus (CoV), designated severe acute respiratory syndrome (SARS)-CoV-2, caused an international outbreak of a respiratory illness (COVID- 19) , and rapidly evolving into a pandemic. Most cases are asymptomatic or self-limiting, but the clinical spectrum of the disease extends to severe progressive pneumonia with acute respiratory distress syndrome (ARDS), which is a life-threatening condition requiring mechanical ventilation and intensive care support.

In a yet to be defined percentage of cases, after about one week, there is a sudden and unpredictable worsening of clinical conditions, properly having as a target the respiratory district. In the first phase of the infection, when the viral replication plays a pivotal pathogenetic role, the use of antiviral drugs could be of the utmost importance in inhibiting SARS-CoV-2 replication and the viral-induced organ damage; unfortunately, to date there are no antiviral therapies specific for COVID- 19 .

Some antivirals initially developed as treatment for human immunodeficiency virus (HIV), including lopinavir/ritonavir association (LPV/r), have been investigated in the past two decades (drug repurposing) for other coronaviruses responsible for serious diseases such as the severe acute respiratory syndrome (SARS) and the Middle East respiratory syndrome (MERS) [1, 2] . In a recent meta-analysis aimed at evaluating the efficacy and safety of current options for SARS and MERS besides COVID-19, the LPV/r-based combinations showed better virological eradication and radiological improvement, with a reduced rate of ARDS as compared with other anti-coronavirus agents [3] . In the absence of proven effective treatments, LPV/r has, thus, been widely used to face the COVID-19 pandemic from the beginning [4] , and is currently investigated in several clinical trials [5] , such as the Solidarity trial launched on 20 March by the World Health Organization [6] .

The aim of this paper is to review the available evidence on the efficacy of LPV/r in COVID-19, SARS, and MERS, and to analyze the current guideline recommendations of the main international scientific societies and agencies on the use of this antiviral drug.

A literature search was performed up to 15 May 2020 through PubMed. The following terms were searched in different combinations: COVID-19, SARS-CoV-2, SARS, MERS, coronavirus, lopinavir, and ritonavir. Variations of these terms were also searched. The selection was limited to articles written in English and published in peer-reviewed journals only. After deduplication, all authors independently screened titles and abstracts, and finally full texts, to identify all potentially relevant papers, resolving discrepancies through discussion and consultation among them. References of retrieved articles were manually searched to ensure identification of relevant studies not found in the initial literature search.

The guideline documents of the main scientific societies involved in the management of COVID-19, and of international agencies, were directly searched and retrieved through direct consultation of their websites, in addition to PubMed searching.

Finally, a search was performed on https://clinicaltrials.gov for the studies regarding the use of lopinavir/ritonavir in COVID-19, in progress or waiting to begin, or completed but not yet published. Figure 1 shows the flow diagram of the literature selection process to identify clinical and laboratory studies regarding LPV/r use in COVID-19, SARS, and MERS. Thirty-seven studies were included for the review. Thirteen documents released by some authoritative scientific societies and international agencies involved in the management of COVID-19 were retrieved. 

Lopinavir (LPV) is an antiretroviral protease inhibitor used in combination with ritonavir (booster) in HIV infection therapy and prevention. LPV is a peptidomimetic HIV type 1 aspartate protease inhibitor that acts by binding to its catalytic site, thereby, preventing the cleavage of viral polyprotein precursors into mature, functional proteins that are necessary for viral replication. LPV is usually given in combination with low booster doses of ritonavir which improves the pharmacokinetics of LPV by slowing its hepatic metabolism through the inhibition of cytochrome P450 3A4 enzyme.

The standard recommended dosage of LPV in adults is 800 mg daily in combination with 200 mg of ritonavir, usually in two divided doses.

Some degree of serum aminotransferase elevations occurs in a high proportion of patients within one to eight weeks, usually asymptomatic and self-limiting with continuation of the medication; however, fatal cases have been reported [7] . Comprehensive additional information about LPV/r can be found at the website https://www.uptodate.com/contents/lopinavir-and-ritonavir-druginformation. 

Lopinavir (LPV) is an antiretroviral protease inhibitor used in combination with ritonavir (booster) in HIV infection therapy and prevention. LPV is a peptidomimetic HIV type 1 aspartate protease inhibitor that acts by binding to its catalytic site, thereby, preventing the cleavage of viral polyprotein precursors into mature, functional proteins that are necessary for viral replication. LPV is usually given in combination with low booster doses of ritonavir which improves the pharmacokinetics of LPV by slowing its hepatic metabolism through the inhibition of cytochrome P450 3A4 enzyme.

The standard recommended dosage of LPV in adults is 800 mg daily in combination with 200 mg of ritonavir, usually in two divided doses.

Some degree of serum aminotransferase elevations occurs in a high proportion of patients within one to eight weeks, usually asymptomatic and self-limiting with continuation of the medication; however, fatal cases have been reported [7] . Comprehensive additional information about LPV/r can be found at the website https://www.uptodate.com/contents/lopinavir-and-ritonavir-drug-information.

LPV/r was developed for inhibition of HIV protease, whose main difference with respect to the SARS-CoV-2 counterpart (3CL pro ) lies within the divergent spatial structure of the HIV aspartic protease as compared with 3CL pro cysteine protease. This would affect its inhibition efficiency [8] .

Recently, it has been pointed out by Baldelli et al. [9] that to establish the optimal dosage of LPV/r in COVID-19 could be very relevant, although it has been completely overlooked so far: in 21 patients concomitantly treated with hydroxychloroquine, all the LPV therapeutic drug monitoring (TDM) resulted in values above the therapeutic range, and the TDM data analysis showed that the COVID-19 patients had trough LPV concentrations three-fold higher as compared with the HIV patients. Virtually all samples exceeded the threshold concentration of 7000 ng/mL, notoriously associated with scarce tolerability in HIV patients. The high concentrations both of LPV and ritonavir could be explained by the SARS-CoV-2-induced liver damage, including the altered expression of drug-metabolizing enzymes, or by the potential interaction with hydroxychloroquine. The authors wisely suggest that an investigation is warranted for a reduced dose of LPV/r (i.e., 400/100 mg daily) to improve drug tolerability in COVID-19 [9] .

The ability of LPV to inhibit the SARS-CoV main protease (3CL pro ) has been evaluated in vitro [10] . No clinical trials were found addressing the efficacy of antiviral agents in the management of SARS-CoV [11] .

Two observational studies reported outcomes in patients who were given LPV/r. In a retrospective matched cohort study conducted in Hong Kong [12] , the addition of LPV/r as initial treatment in 44 patients was associated with a reduction of the overall death rate (2.3%) and intubation rate (0%) as compared with a matched cohort of 634 patients who received standard treatment (15.6% and 11.0% respectively, p < 0.05) and a lower rate of use of methylprednisolone at a lower mean dose. The subgroup of 31 patients, who received LPV/r as a rescue therapy, showed no difference in overall death rate and rates of oxygen desaturation and intubation as compared with a matched cohort of 343 patients, and received a higher mean dose of methylprednisolone. In another study [13] , LPV/r was administered in addition to ribavirin to 41 patients. Adverse clinical outcomes (ARDS or death) at 21 days were significantly lower than in 111 historical controls treated with ribavirin only (2.4% vs. 28.8%, p < 0.001) three weeks after the onset of symptoms, and this positive effect was shown in those diagnosed both early and later in the course of the epidemic. A reduction in steroid usage and nosocomial infections and decreasing viral loads were seen in patients initially treated with LPV/r. Focusing on multivariate analysis, the lack of treatment with this antiviral was an independent predictor of adverse outcomes. LPV showed in vitro antiviral activity at 48 h at concentrations of 4 µg/mL.

However, both these studies were determined to be "inconclusive" due to the possible bias in the selection of the control group or treatment allocation [14] .

In an in vitro study [15] , LPV inhibited MERS-CoV-induced cytopathic effect with a 50% effective concentration (EC 50 ) of 8 µM, and a maximal protective effect (89% inhibition) was observed at a dose of 12 µM. These values are in the range of the LPV plasma concentrations (8 to 24 µM) observed in HIV patients with acquired immune deficiency syndrome (AIDS).

No published clinical trials were found addressing the efficacy of antiviral agents in the management of MERS-CoV [11] .

From May to July 2015, the Republic of Korea experienced the largest outbreak of MERS outside the Arabian Peninsula: a retrospective observational study focused on the clinical characteristics of confirmed MERS cases [16] . An antiviral therapy was administered to 138/186 patients, within a median time of six days from the onset of illness, and LPV/r was commonly prescribed to 86.6% of patients, usually in combination with interferon and ribavirin (81.1%) or ribavirin only (5%), and as a monotherapy in 0.8% only. Since the case fatality rate observed in this study was lower than that reported in other studies of previous MERS outbreaks (20.4% vs. 36.5-65%), the authors suggested that this low rate could be attributed to the application of more aggressive treatment measures, including the antiviral agents.

In a nonhuman primate model (common marmoset) of MERS, animals treated with LPV/r and interferon-β 1b had a better outcome than the untreated, with improved clinical, radiological, and pathological findings, and lower mean viral loads in lung and extra-pulmonary tissues [17] .

The MIRACLE (MERS-CoV Infection tReated with A Combination of Lopinavir/ritonavir and intErferon-β 1b, ClinicalTrials.gov ID NCT02845843) [18] is a multicenter double-blind randomized placebo-controlled trial (RCT) that is currently recruiting patients to investigate the efficacy (the primary outcome is 90-day mortality) of this combination therapy in hospitalized patients. The MIRACLE trial is the first RCT performed for MERS treatment.

The Public Health England recommendations on "Treatment of MERS-CoV" stated that "LPV may be considered for specific treatment of MERS patients ( . . . ), routinely available ( . . . ), likely to be the most accessible treatment initially ( . . . ), well-established agent with favorable toxicity profile. Gastrointestinal side effects are common but self-limiting" [19] .

Crystal structure of SARS-CoV-2 protease has been released, providing the structural basis for identification of drugs that could interact with this target. Computer-aided drug design can play an essential role to identify new active drugs. LPV displayed inhibitory activities against SARS-CoV-2 main protease [20] . The role of the nonstructural protein of coronaviruses, main protease, or 3C-like proteases (3CL pro ), involves the proteolytic processing of the replicase polyprotein, and is crucial for viral replication and maturation; this protease shares a similar common cleavage site among coronaviruses, and the sequence alignment of SARS-CoV-2 3CL pro shows a 96.1% identity as compared with that of SARS-CoV. Coronavirus 3CL pro is considered to be an attractive drug target for the treatment of coronavirus infections. Both LPV and ritonavir effectively interact with the residues at the active site of SARS-CoV-2 3CL pro . Ritonavir shows a somewhat higher number of atomic contacts, a somewhat higher binding efficiency, and a somewhat higher number of key binding residues as compared with LPV, which corresponds with the slightly lower water accessibility at the 3CL pro active site [21] .

A recent study [22] showed that both remdesivir and LPV (but not ritonavir) inhibited SARS-CoV-2 replication in Vero E6 cells, with the estimated EC 50 at 23.15 and 26.63 µM, respectively, while other compounds currently undergoing clinical trials (such as ribavirin, favipiravir, oseltamivir, or baloxavir) showed no apparent in vitro antiviral effect at concentrations under 100 µM.

In the first retrospective single-center study describing the clinical characteristics of 98 hospitalized COVID-19 patients in South Korea, 99% of the patients received LPV/r [23] , as well as 82% of the critically ill patients hospitalized in Brescia, Italy [24] , testifying how this antiviral drug has been widely used in clinical practice, worldwide, to face this dramatic illness.

Wu et al. [25] evaluated risk factors for ARDS in 201 COVID-19 patients, most of whom (84.6%) received different antiviral drugs, including LPV/r (14.9%). Patients who developed ARDS were less likely to be treated with antiviral therapy (difference, −14.4%, 95% CI, −26.0% to −2.9%, p = 0.005), and the same occurred in those who died (difference, −40.7%, 95% CI, −58.5% to −22.9%, p < 0.001). However, the low number of patients treated with LPV/r did not allow them to make any conclusion on the efficacy of this drug.

LPV/r has been reported to be associated with faster resolution of fever, with no evident toxicity and only low side effects (mainly nausea, vomiting, and diarrhea), and with fewer days for SARS-CoV-2 RNA detection turning negative [26] . It has been suggested that LPV/r can reduce viral loads [27] , and that the discontinuation of antiviral drugs, including LPV/r, could be the reason for recovered COVID-19 patients testing positive again, with new worsening of pulmonary damage [28] . However, it has also been shown that LPV/r did not shorten the duration of SARS-CoV-2 shedding in patients with mild pneumonia [29] . It has been reported a significantly more elevated negative conversion rate of coronavirus test in seven days and 14 days, and a significant improvement of chest radiological findings in seven days, when LPV/r was administered in combination with oral arbidol [30] . In another retrospective study, LPV/r (400/100 mg twice a day for one week) was reported to be inferior to arbidol in terms of viral load reduction and duration of positive RNA testing [31] .

A specific focus on LPV/r administration was done in a descriptive case series of the first 18 patients diagnosed in Singapore. Five patients requiring supplemental oxygen were treated with LPV/r, but the evidence of clinical benefit was equivocal, since defervescence and reduction of supplemental oxygen occurred in three patients within one to three days of LPV/r initiation, but it was unable to prevent the progression of the disease in the remaining two patients. In addition, 4/5 patients developed nausea, vomiting, or diarrhea, and three patients developed an abnormal liver function test. A decline in viral load in nasopharyngeal swabs also appeared to be similar between treated and untreated patients [32] .

The efficacy of LPV/r has been specifically investigated in a randomized controlled open-label trial by Cao et al. [33] , in which 99 patients with severe COVID-19 were randomized to receive LPV/r (400/100 mg twice a day) and 100 patients to standard of care, for 14 days. LPV/r administration was not associated with a statistically significant difference in the time to clinical improvement (the primary outcome), although in the modified intention-to-treat analysis, excluding three patients who died within 24 h and who never received the medication, the between-group difference (median, 15 days vs. 16 days) was significant, albeit modest. Moreover, the median time when the patients participated in the study was 13 days after symptom onset, when they had already progressed to a very severe condition (not excludable, being secondary to virus-induced systemic inflammatory response due to cytokine release syndrome). In a post-hoc subgroup analysis, the difference in mortality between the LPV/r group and the standard-care group was observed to be numerically greater among patients treated within 12 days after the onset of symptoms than among those treated later. In addition, in the LPV/r group as compared with the standard-care control group: the 28-day mortality was lower (19.2% vs. 25%, but the difference was not statistically significant), patients presented a shorter stay in the intensive care unit (median, six days vs. 11 days), the duration from randomization to hospital discharge was numerically shorter (median, 12 days vs. 14 days), the percentage of patients with clinical improvement at day 14 was higher (45.5% vs. 30.0%), the risk of respiratory failure or ARDS was lower (12.6% vs. 27.3%), secondary infections were lower (1.1% vs. 6.1%); moreover, in the LPV/r group as compared with the standard-care control group, a lower use of vasopressors (17.2% vs. 27.0%), renal-replacement therapy (3.0% vs. 6.0%), noninvasive (10.1% vs. 19.0%) and invasive (14.1% vs. 18.0%) mechanical ventilation was reported. The viral RNA load or duration of viral RNA detectability did not differ between the two groups. LPV/r was associated with more adverse events, in particular gastrointestinal adverse events, including anorexia (2.1%), nausea (9.5%), abdominal discomfort (4.2%), vomiting (6.3%), or diarrhea (4.2%), as well as two serious adverse episodes of acute gastritis. Increased levels of transaminases were instead less frequently reported in the LPV/r group than in the controls. This was not a blinded trial, and the small population enrolled was the main limitation of this trial; it was likely that if the RCT had been larger, some of the favorable point estimates could have reached statistical significance. Moreover, the enrolled population had severe disease (overall mortality of 22%), and this could have contributed to the poor effect associated with the treatment; this highlights the importance of an early antiviral approach when in the pathogenesis of COVID-19 the "viral replication phase" prevails over the "host immune response". Finally, the somewhat higher throat viral loads in the LPV/r group raise the possibility that this group had more viral replication.

After the publication of this RCT, many clinicians stopped using LPV/r, with some scientific societies even recommending against its use.

Many authors suggested a different reading and alternative analyses of the results of this trial. It was highlighted by Corrao et al. [34] that even if the results of a trial have no statistical significance, signals are important if the sample size is small, and no strong conclusions can be made until a trial with the correct sample size has been performed. Carmona-Bayonas et al. [35] reanalyzed the data of Cao et al. [33] with a Bayesian Cox proportional hazards model and showed that there was a 73% posterior probability of a clinical improvement of more than 15% and a 17% probability that the effect was in a region of practical equivalence. Since this trial was underpowered, the results did not sustain the conclusion that LPV/r was ineffective. Cao et al. [36] recently admitted that on the basis of the results regarding different outcomes and alternative data analyses, LPV/r could still be a potential therapeutic agent against COVID-19, and wisely recommended that clinicians review all the data about all the outcomes in their trial before making any clinical decisions regarding treatment.

A recent multicenter, prospective, open-label, randomized, phase II trial [37] showed that 86 hospitalized patients early assigned (within a median of five days) to a 14 day triple combination of LPV/r 400/100 mg every 12 h, ribavirin 400 mg every 12 h, and three doses of 8 million international units of interferon-β 1b on alternate days, had a significantly shorter median time from start of treatment to negative nasopharyngeal swab as compared with a control group of 41 patients treated only with LPV/r for 14 days (7 days vs. 12 days, p = 0.0010). In addition, the triple combination also alleviated symptoms completely within four days. The significantly better clinical and virological response was also reflected by the shorter median hospital stay in the combination group than in the control group (9 days vs. 14.5 days, p = 0.016).

A meta-analysis [38] recently concluded that treatment with LPV/r had no significant benefit in mortality and ARDS rates in COVID-19 patients, but, on subgroup analysis, the LPV/r group had a lower rate of ARDS, although this difference was not statistically significant (15.6% vs. 24.2%, p = 0.49). It is noteworthy that all included studies in this meta-analysis were observational, since the Cao's RCT [33] was published after this search was conducted 3.6. Guideline Recommendations for LPV/r in COVID-19 Table 1 shows a synthesis of the guideline recommendations issued by the main scientific societies and agencies about LPV/r use in COVID-19. We suggest not using LPV/r in patients with non-severe and severe COVID- 19 Weak recommendation GRADE approach Against SSC, 2020 [40] In critically ill adults with COVID-19 we suggest against the routine use of LPV/r Weak recommendation, low-quality evidence GRADE approach Against SITA, SIP, 2020 [41] At the present time, evidence from the first published RCT does not support off-label treatment with LPV/r in COVID-19 patients

One randomized trial Consensus Against/Uncertain NIH, 2020 [42] There are insufficient data to recommend either for or against the use of any antiviral or immunomodulatory therapy in patients with COVID-19 who have mild, moderate, severe, or critical illness (AIII). Except in the context of a clinical trial, the Panel recommends against the use of LPV/r because of unfavorable pharmacodynamics and negative clinical trial data (AI).

A: Strong recommendation I: One or more randomized trials III: Expert opinion Consensus Against/Uncertain WHO, 2020 [43] There is no current evidence to recommend any specific anti-COVID-19 treatment for patients with confirmed COVID-19. There are many ongoing clinical trials testing various potential antivirals.

DGIIN, DIVI, DGP, DGAI, 2020 [44] We recommend to only use LPV/r (and other drugs) as part of compassionate use programs or approved study protocols after carefully evaluating risks and benefits for the individual patient

Consensus, multidisciplinary approach Uncertain Table 2 shows a summary of the numerous ongoing interventional trials around the world investigating the efficacy of LPV/r in COVID-19 (available online at https://clinicaltrials.gov, accessed on 15 May 2020). 

To date, available evidence about the efficacy and the effectiveness of LPV/r in COVID-19 is poor and generally of low quality. There is only one RCT of adequate methodology conducted to address the topic whether adding LPV/r to the standard of therapy can bring clinical benefits [33] , but, as previously discussed, the results should be read with great attention given the limited size of the enrolled sample; however, this RCT represents a research milestone for COVID-19, which demonstrates how in these dramatic pandemic times the scientific method can still be maintained. Another RCT recently published [37] has instead explored a different point of view, considering LPV/r as the standard of therapy (control group), and showed that the addition of ribavirin and interferon-β 1b to LPV/r confers clinical benefits.

Many scientific societies and agencies have used the GRADE approach and the consensus method to release their guidelines, and the recommendations have sometimes been expressed as "expert opinion". Rightly, the results of the RCT of Cao et al. [33] are generally held in very high regard, despite several limits of this study, but our impression is that they "obscured" the data that emerged from several other studies, even if of lower quality, and from the very extensive clinical experience that has been made on the use of LPV/r from the beginning of the COVID-19 pandemic, with the efficacy of all alternative treatments still needing proofs.

Often the "net balance of recommendation" is uncertain, and LPV/r is recommended only in the context of a clinical trial. It should also be remembered that numerous ongoing interventional trials around the world are currently evaluating the efficacy of LPV/r in COVID- 19. In some cases, a recommendation clearly against the use has been expressed [39, 40] , in other cases it resulted more favorably [48] [49] [50] [51] . In the past, the Public Health England has recommended LPV as a possible option for MERS patients, for its routinely availability and well-established favorable toxicity profile [19] , even in the absence of strong evidence about the efficacy. Lacking to date effective treatment for COVID-19, and pending results of ongoing RCTs, in our opinion the same rational considerations of the favorable benefit/risk balance could also be prudently made for COVID-19.

We are fully aware of the seriousness of the current COVID-19 pandemic, and the lack of therapies of proven efficacy should in no way legitimize a failure of the scientific method. The validity of a given therapy must be properly demonstrated, but this applies both to its definitive approval and rejection. Consideration which are too hasty could have serious consequences.

In our opinion, at the current time, clinicians should not abandon the use of LPV/r for the treatment of COVID-19, pending results of numerous ongoing trials evaluating the efficacy of this drug.

Author Contributions: All authors made substantial contributions to the conception of the work, acquisition and interpretation of data, and in drafting the work; all authors approved the submitted version. All authors have read and agreed to the published version of the manuscript.

Funding: This research received no external funding.

The authors declare no conflict of interest.

A systematic review of lopinavir therapy for SARS coronavirus and MERS coronavirus-A possible reference for coronavirus disease-19 treatment option

Systematic review of the efficacy and safety of antiretroviral drugs against SARS, MERS or COVID-19: Initial assessment

Efficacy and safety of current therapeutic options for COVID-19 -lessons to be learnt from SARS and MERS epidemic: A systematic review and meta-analysis

Drug treatment options for the 2019-new Coronavirus (2019-nCoV)

Solidarity" Clinical Trial for COVID-19 Treatments

LiverTox: Clinical and Research Information on Drug-Induced Liver Injury

SARS-CoV-2: Recent reports on antiviral therapies based on Lopinavir/Ritonavir, Darunavir/Umifenovir, Hydroxychloroquine, Remdesivir, Favipiravir and other drugs for the treatment of the new coronavirus

Lopinavir/ritonavir in COVID-19 patients: Maybe yes, but at what dose?

Small molecules targeting severe acute respiratory syndrome human coronavirus

Antiviral therapy in management of COVID-19: A systematic review on current evidence

Treatment of severe acute respiratory syndrome with lopinavir/ritonavir: A multicentre retrospective matched cohort study

Role of lopinavir/ritonavir in the treatment of SARS: Initial virological and clinical findings

Systematic review of treatment effects

Screening of an FDA-approved compound library identifies four small-molecule inhibitors of Middle East respiratory syndrome coronavirus replication in cell culture

Clinical presentation and outcomes of Middle East Respiratory Syndrome in the Republic of

Treatment with Lopinavir/Ritonavir or Interferon-β1b improves outcome of MERS-CoV infection in a nonhuman primate model of common marmoset

Treatment of Middle East Respiratory Syndrome with a combination of lopinavir-ritonavir and interferon-β1b (MIRACLE trial): Study protocol for a randomized controlled trial

Treatment of MERS-CoV: Information for Clinicians. Clinical Decision-Making Support for Treatment of MERS-CoV Patients

Fast identification of possible drug treatment of Coronavirus Disease -19 (COVID-19) through computational drug repurposing study

Why are Lopinavir and Ritonavir effective against the newly emerged coronavirus 2019? Atomistic insights into the inhibitory mechanisms

Remdesivir, lopinavir, emetine, and homoharringtonine inhibit SARS-CoV-2 replication in vitro

Clinical Features and Outcomes of 98 Patients Hospitalized with SARS-CoV-2 Infection in Daegu, South Korea: A Brief Descriptive Study

Clinical presentation and initial management critically ill patients with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection in Brescia

Risk Factors Associated With Acute Respiratory Distress Syndrome and Death in Patients With Coronavirus Disease

Clinical efficacy of lopinavir/ritonavir in the treatment of Coronavirus disease 2019

Case of the index patient who caused tertiary transmission of COVID-19 Infection in Korea: The Application of Lopinavir/Ritonavir for the Treatment of COVID-19 Infected Pneumonia Monitored by Quantitative RT-PCR

Discontinuation of antiviral drugs may be the reason for recovered COVID-19 patients testing positive again

Lopinavir/ritonavir did not shorten the duration of SARS CoV-2 shedding in patients with mild pneumonia in Taiwan

Arbidol combined with LPV/r versus LPV/r alone against Corona Virus Disease 2019: A retrospective cohort study

Arbidol monotherapy is superior to lopinavir/ritonavir in treating COVID-19

Epidemiologic Features and Clinical Course of Patients Infected With SARS-CoV-2 in Singapore

A Trial of Lopinavir-Ritonavir in Adults Hospitalized with Severe Covid-19

A Trial of Lopinavir-Ritonavir in Covid-19

A Trial of Lopinavir-Ritonavir in Covid-19

A Trial of Lopinavir-Ritonavir in Covid-19

Triple combination of interferon beta-1b, lopinavir-ritonavir, and ribavirin in the treatment of patients admitted to hospital with COVID-19: An open-label, randomised, phase 2 trial

Risk Factors of Severe Disease and Efficacy of Treatment in Patients Infected with COVID-19: A Systematic Review, Meta-Analysis and Meta-Regression Analysis

Treatment of patients with nonsevere and severe coronavirus disease 2019: An evidence-based guideline

Surviving Sepsis Campaign: Guidelines on the Management of Critically Ill Adults with Coronavirus Disease 2019 (COVID-19)

Balancing evidence and frontline experience in the early phases of the COVID-19 pandemic: Current position of the Italian Society of anti-infective therapy (SITA) and the Italian Society of Pulmonology (SIP)

19 Treatment Guidelines

Clinical Management of Severe Acute Respiratory Infection (SARI) When COVID-19 Disease Is Suspected. Interim Guidance 13

German Recommendations for Critically Ill Patients with COVID-19

COVID-19: Interim Guidance on Management Pending Empirical Evidence. From an American Thoracic Society-led International Task Force

Infectious Diseases Society of America Guidelines on the Treatment and Management of Patients with COVID-19

Evidence-Based Medicine Chapter of China International Exchange and Promotive Association for Medical and Health Care (CPAM). A rapid advice guideline for the diagnosis and treatment of 2019 novel coronavirus (2019-nCoV) infected pneumonia (standard version)

Interim Guidelines on Antiviral Therapy for COVID-19

Diagnosis and Treatment Protocol for COVID-19 (Trial Version 7) issued by the General Office of the National Health Commission and the Office of the National Administration of Traditional Chinese Medicine

SIMIT Vademecum Per La Cura Delle Persone Con Malattia Da COVI-19. Versione 2.0