Abstract
Introduction
Guidelines for treatment of multidrug-resistant (MDR) bacteria rely on newly approved antibiotics, with limited evidence of their effectiveness for treating these infections. Data regarding cost of such an approach are lacking. We aimed to evaluate estimated cost of using newly approved antibiotic drugs compared to older antibiotics for the treatment of difficult-to-treat pathogens.
Methods
MDR bacteria of interest included those defined by the World Health Organization as critical or of high priority for research. Old and newly approved antibiotics for these bacteria, defined as approved before or after January 2010, respectively, were evaluated for treatment cost and for 14-day treatment course. Estimated annual costs were calculated based on the Centers for Disease Control and Prevention’s' report on MDR bacteria prevalence in US hospitalized patients. Old and new drugs costs were compared.
Results
The cost of a 14-day treatment course for methicillin-resistant Staphylococcus aureus bacteremia with a newly approved drug was found to be 6 to 60 times higher than that of older drugs. Similarly, the cost of a 14-day course for carbapenem-resistant Enterobacterales or MDR Pseudomonas aeruginosa was doubled with new drugs; and for carbapenem-resistant Acinetobacter baumannii, ~ 20 times higher with newer drugs. Annual incremental costs of treating difficult-to-treat Gram-negative bacteria with new drugs ranged from 30 million to over 500 million USD.
Conclusions
Using newly approved antibiotic drugs for MDR infections carries a large incremental cost. Additional data to support survival benefit of these drugs are required to justify the price differences. Subgroups of patients who would benefit most from treatment should be defined.
Supplementary Information
The online version contains supplementary material available at 10.1007/s40121-021-00412-y.
Keywords: Antibiotics, Costs analysis, Guidelines, MDR
Key Summary Points
| Why carry out this study? |
| Guidelines for treatment of multidrug-resistant (MDR) bacteria rely on newly approved antibiotics. |
| We aimed to assess how much would it cost to base treatment for multidrug-resistant bacterial infections on those new antibiotics. |
| What was learned from the study? |
| Annual incremental cost of new antibiotics could reach 30–500 million USD for some bacteria. |
| Lack of solid evidence for superior effectiveness of new antibiotics for these bacteria complicates treatment decisions. |
| Cost should be part of the discussion while considering use of newly approved antibiotics until further evidence for effectiveness accumulates. |
Digital Features
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Introduction
Multidrug-resistant (MDR) bacterial infections are a growing problem worldwide. According to a recent Centers for Disease Control and Prevention (CDC) report, over 2.8 million cases of antibiotic-resistant infections occur annually in the US, resulting in over 35,000 deaths [1]. In addition to the medical challenges posed by these infections, they also constitute a public health and economic burden. The spending for one MDR infection has been reported to be 165% higher than for non-MDR infection, with an incremental cost of 1383 USD. This has been translated to a national annual cost of 2.2 billion USD in 2014, mostly attributed to antibiotic costs [2, 3].
Recently, the Infectious Diseases Society of America (IDSA) issued guidelines for treatment of antimicrobial-resistant Gram-negative bacteria. Newly approved drugs dominate treatment recommendations in these guidelines, although their effectiveness for specific MDR infections is supported by limited evidence for survival benefit [4, 5].
We aimed to evaluate the estimated cost of using newly approved antibiotics compared to old antibiotics for the treatment of specific difficult-to-treat pathogens.
Methods
We searched the US Food and Drugs Administration (FDA) website for antibacterial drugs with in vitro activity against specific MDR ESKAPE bacteria [vancomycin-resistant Enterococcus faecium (VRE), methicillin-resistant Staphylococcus aureus (MRSA), carbapenem-resistant Klebsiella pneumoniae, carbapenem-resistant Acinetobacter, MDR Pseudomonas aeruginosa, and carbapenem-resistant Enterobacter spp.) [6]. ESKAPE pathogens were chosen as bacteria of interest based on World Health Organization definition of these bacteria as critical or high priority for research and drug development [7]. Drugs approved between 1 January 2010 and 14 November 2020 were included, and were considered “new” [6]. For each resistant pathogen, we created a list of potentially covering antibiotics, divided into "old" and "new" according to approval before and after 1 January 2010, respectively [4, 6, 8]. Drugs not approved for use in the US were excluded (teicoplanin, intravenous fosfomycin). For each drug, the cost per day and for a 14-day treatment course were determined using the IBM Micromedex Red Book website [9]. The annual price of treating each bacteria using its individual drug options was calculated by multiplying the cost of a 14-day treatment course and the estimated number of annual infections, as detailed in the recent CDC report [1] (see details regarding cost calculation in Supplement 1). Ethical approval was not required for this study, as data were collected from public databases.
Results
The list of included bacteria, their relevant "old" and "new" drugs, and daily costs are provided in Table 1.
Table 1.
Included bacteria, relevant "old" and "new" drugs, dosages, and costs
| Bacteria name | Estimated number of cases in the US in hospitalized patients (2017) | Old antibiotic drugs | New antibiotic drugs | ||||||
|---|---|---|---|---|---|---|---|---|---|
| Drug name | Dose | Cost per treatment course (USD)a | Estimated annual cost (USD) | Drug name | Dose | Cost per treatment course (USD)a | Estimated annual cost (USD) | ||
| Vancomycin-resistant Enterococcus faecium (VRE) | 54,500 | Daptomycin |
8-10 mg/kg × 1/day (~ 750 mg × 1/day) |
1093 | 59,544,520 | Omadacycline |
IV: loading 200 mg; Maintenance 100 mg × 1/day O: 300 mg × 1/day |
IV: 6200 PO: 6951 |
IV: 337,900,000 PO: 378,829,500 |
| Linezolid | 600 mg × 2/d | 2188 | 119,226,380 | ||||||
| Tigecycline | Loading: 200 mg; Maintenance: 100 mg × 2/day | 6989 | 380,889,600 | Oritavancin | 1200 mg (Single dose) | 2987 | 162,791,500 | ||
| Telavancin |
10 mg/kg × 1/day (~ 750 mg × 1/day) |
8595 | 468,443,850 | ||||||
| Methicillin-resistant Staphylococcus aureus (MRSA) | 323,700 | Vancomycin | 15 mg/kg × 2/day (~ 1 gr × 2/day) | 115 | 37,225,500 | Ceftaroline | 600 mg × 2/day | 6778 | 2,194,038,600 |
| Daptomycin |
8-10 mg/kg × 1/day (~ 750 mg × 1/day) |
1093 | 353,804,100 | Dalbavancin |
1,000 mg (single dose) + 500 mg (1 week later) |
5691 | 1,842,176,700 | ||
| Linezolid | 600 mg × 2/d | 2188 | 708,255,600 | Oritavancin | 1200 mg (Single dose) | 2987 | 966,891,900 | ||
| Telavancin | 10 mg/kg × 1/day (~ 750 mg × 1/day) | 8595 | 2,782,201,500 | Tedizolid | 200 mg × 1/day | 5170 | 1,673,529,000 | ||
| Lefamulin |
IV: 150 mg × 2/day PO: 600 mg × 2/day |
IV: 3444 PO: 4620 |
IV: 1,114,822,800 PO: 1,495,494,000 |
||||||
| Delafloxacin |
IV: 300 mg × 2/day PO: 450 mg × 2/day |
IV: 4452 PO: 2380 |
IV: 1,441,112,400 PO: 770,406,000 |
||||||
| Omadacycline |
IV: loading 200 mg, maintenance 100 mg × 1/day PO: 300 mg × 1/day |
IV: 6200 PO: 6951 |
IV: 2,006,940,000 PO: 2,250,038,700 |
||||||
| Carbapenem-resistant Enterobacterales | 13,100 | Meropenem | 2 g × 3/day | 717 | 9,392,700 | Ceftazidime-avibactam | 2.5 g × 3/day | 18,084 | 236,900,400 |
| Colistimethate | Loading: 9 MU (~ 300 mg); Maintenance: 4.5 MU × 2/day (~ 150 mg × 2/day) | 941 | 12,327,100 | Meropenem-Vaborbactam | 4 g × 3/day | 16,632 | 217,879,200 | ||
| Amikacin | 15 mg/kg × 1/day (~ 1 gr × 1/day) | 260 | 3,406,000 | Cilastatin / Imipenem / Relebactam |
1.25 g × 4/day |
17,976 | 235,485,600 | ||
| Gentamicin | 240 mg × 1/day | 44 | 576,400 | Cefiderocol | 2 g × 3/day | 18,480 | 242,088,000 | ||
| Tigecycline |
Loading: 200 mg once; Maintenance: 100 mg × 2/day |
6989 | 91,555,900 | Eravacycline |
1 mg/kg × 2/day (~ 100 mg × 2/day) |
3293 | 43,138,300 | ||
| Plazomicin | 15 mg/kg × 1/day (~ 1000 mg × 1/day) | 10,584 | 138,650,400 | ||||||
| Carbapenem-resistant Acinetobacter baumannii (CRAB) | 8500 | Colistimethate |
Loading: 9 MU (~ 300 mg); Maintenance: 4.5 MU × 2/day (~ 150 mg × 2/day) |
941 | 7,998,500 | Cefiderocol | 2 g × 3/day | 18,480 | 157,080,000 |
| Minocycline | 100 mg × 2/day | 5448 | 46,308,000 | ||||||
| Tigecycline |
Loading: 200 mg once; Maintenance: 100 mg × 2/day |
6989 | 59,406,500 | ||||||
| Meropenem | 2 g × 3/day | 717 | 6,094,500 | ||||||
|
Multidrug-resistant Pseudomonas aeruginosa |
32,600 | Gentamicin | 240 mg × 1/day | 44 | 30,676,600 | Ceftazidime-avibactam | 2.5 g × 3/day | 18,084 | 589,538,400 |
| Amikacin | 15 mg/kg × 1/day (~ 1 gr × 1/day) | 260 | 8,476,000 | Ceftolozane-tazobactam |
HAP/VAP: 3 g × 3/day UTI: 1.5 g × 3/day |
HAP/VAP: 12,628 UTI: 6314 |
HAP/VAP: 411,672,800 UTI: 205,836,400 |
||
| Colistimethate |
Loading: 9 MU (~ 300 mg); Maintenance: 4.5 MU × 2/day (~ 150 mg × 2/day) |
941 | 1,434,400 | Cefiderocol | 2 g × 3/day | 18,480 | 602,448,000 | ||
| Cilastatin / Imipenem / Relebactam |
1.25 g × 4/day |
17,976 | 586,017,600 | ||||||
HAP Hospital-acquired pneumonia, IV intravenous, PO Pers. ob., UTI urinary tract infection, VAP ventilator-associated pneumonia
aAll treatment costs were calculated for a 14-day treatment course, unless mentioned otherwise
For VRE, the most commonly used old drug cost for a 4-day treatment course ranged between 1093 USD (daptomycin) and 2188 USD (linezolid), and reached up to 6989 USD (tigecycline) and 8595 USD (telavancin). New drug options for VRE are limited, and include omadacycline (6200 USD per course), and oritavancin (2987 USD per course of one dose).
For MRSA bacteremia, a 14-day course of the new drug ceftaroline would cost over six times more than a course of daptomycin (6778 vs. 1093 USD), and ~ 60 times the cost of 14 days of vancomycin, the current first-line treatment for these infections [10]. For other sources of infection, the costs of old drugs are also significantly lower for MRSA pneumonia, with 14 days of ceftaroline or lefamulin treatment costing at least 2–3 times more than for linezolid and 40–60 times than for vancomycin, while, for skin and soft tissue infections, clindamycin, trimethoprim-sulfamethoxazole, and doxycycline would have negligible costs compared to lipoglycopeptides, delafloxacin, or omadacycline (Table 1).
For MDR Gram-negative infections, treatment with old drugs is based on various combinations of colistin, tigecycline, meropenem, and aminoglycosides. Recent IDSA guidelines recommend as preferred treatments for carbapenem-resistant Enterobacterales (CRE) and difficult-to-treat Pseudomonas aeruginosa mainly new drugs, including ceftazidime-avibactam, ceftolozane-tazobactam, meropenem-vaborbactam, imipenem-relebactam, and cefiderocol [4]. A treatment course with any of these would cost double that for the colistin-tigecycline combination and ~ 20 times the cost of colistin monotherapy, commonly used for Carbapenem-resistant Acinetobacter baumannii (CRAB) infections [11].
Considering 8500 annual CRAB infections in hospitalized patients [1], treating all of them with cefiderocol instead of colistin would have an annual incremental cost of ~ 150 million USD, 20 times that of colistin, based on randomized controlled trials (RCT) showing increased mortality with the former drug [12]. Similarly, the additional treatment cost of 3100 annual carbapenem-resistant Enterobacteriaceae infections with ceftaizidime-avibactam over the colistin-tigecycline combination would have an incremental cost of ~ 31 million USD, more than doubling the cost. For 32,600 MDR P. aeruginosa annual cases, imipenem-relebactam treatment would cost 577 million USD more than amikacin, 69 times the cost of the older drug.
Discussion
Infections with ESKAPE pathogens are life-threatening, severe infections, carrying substantial mortality. Preventive strategies have accomplished a reduction/stabilization in the number of ESKAPE infections in the US [1]. Yet, highly resistant Gram-negative infections were recently estimated to require between 39 and 138.2 days of therapy for 10,000 patient encounters. In other countries, rates are even higher, with over 10% of Gram-negative bacteremias caused by difficult-to-treat resistant pathogens [13].
Due to the severity and poor outcome of these infections, development of new drugs has been prioritized by policy-makers. Four years after FDA’s approval of ceftazidime-avibactam, new anti-CRE drugs were reported to be used less widely than expected. Explanations suggested for the relatively low uptake (estimated at 35%) include high cost, shortage or non-availability issues, and lack of evidence from RCTs supporting superior efficacy and safety [14]. Ongoing emergence of resistance to these new drugs could also contribute to the restricted use, as well as delays in the availability of susceptibility testing methods [13, 15]. Even with restricted use, annual sales of ceftazidime-avibactam, meropenem-vaborbactam, and plazomicin in 2018–9 were estimated at 101 million USD, while it has been estimated that, with a 100% uptake, the cost would have been 289 million [13].
Recent IDSA guidelines for the treatment of difficult-to-treat Gram-negative infections rely mainly on new antibiotics [4]. Recommendations in these guidelines were based on observational studies and two small RCTs, showing mortality benefit of meropenem-vaborbactam for carbapenem-resistant Enterobacterales infections and imipenem-relebactam for MDR Pseudomonas infections [16]. Cefiderocol, as treatment for carbapenem-resistant Gram-negative bacteria, was demonstrated to result in increased all-cause mortality compared with colistin-based therapy in the only RCT published for this indication [12].
We found that the incremental cost of selecting new drugs over older ones could reach hundreds of millions of USD annually, with limited evidence for superior effectiveness. These costs were calculated for hospitalized patients, not considering the increased burden of such infections in other institutional sites of care, such as nursing homes.
Trials addressing new drugs specifically for highly resistant pathogens are scarce, and the evidence for the use of some of these drugs is sometimes very poor. We found that using the ceftaroline for MRSA bacteremia, which has never been tested in an RCT, would cost 60 times the cost of vancomycin. Nevertheless, Gram-positive infections are less of a problem compared to Gram-negative ones. Many options are available for treating skin and soft tissue infections caused by MDR Gram-positive infections, and the choice of using new drugs may be only for the purpose of oral step-down or the use of single-dose administration. For Gram-negative bacteria, clinicians may face infections that are resistant to all older drugs, since resistance to colistin and meropenem have increased, and the use of new drugs would likely be necessary. Regarding Gram-negative infections, the annual cost of cefiderocol for CRAB infections was estimated to be 20 times that of colistin. The only RCT comparing the two showed increased all-cause mortality with cefiderocol [12, 17]. Trials like the latter, specifically including patients with MDR infections, are difficult to conduct. Their performance involves identifying a sufficient number of patients with a possibly life-threatening infection, and obtaining their consent to receive an old drug perceived to be less effective.
It should be noted that our cost analysis is limited to the situation in the US. Hence, the generalization of our data may be limited, and may depend on the cost of the drugs in other countries, the epidemiology of resistant bacteria, and the availability of new drugs.
The discussion regarding antibiotic cost may change in the near future if the UK’s innovative ‘subscription-type’ payment model gets broad acceptance. In this model, the UK’s National Health Service will pay a bulk sum for an annual payment to pharmaceutical companies, purchasing the whole yearly supply of necessary antibiotics based on the health benefits to patients according to NHS consideration. This will likely negate the need to specifically consider the price of each antibiotic before treating a patient, and is also thought to be able to secure a constant pipeline of new antimicrobials, by providing companies with an upfront payment which can be used in future development ventures. Two antibiotic drugs that were first selected for purchase in this model are cefiderocol and ceftazidime-avibactam [18].
Conclusions
Older drugs have limited effectiveness and some have considerable toxicities [4]. The development of new drugs is of high priority, and their use may provide important benefits for patients, including a survival benefit. Nevertheless, additional proof of such benefits should come from clinical trials, and drug prices should be part of the discussion while considering the use of these drugs. Local protocols regarding antibiotic use should take into account regional costs and the availability of new antibiotics, in addition to the epidemiology of various MDR bacteria. Assessment of the risk of toxicity and/or reduced effectiveness should be conducted on a case-by-case basis prior to decisions on an antibiotic regimen. Subgroups of patients who would benefit most from these new, expensive drugs, should be defined, and include populations often excluded or under-represented in RCTs, e.g., immunocompromised patients, patients with baseline renal dysfunction, and elderly patients. Future studies should include these patients and report results specifically for these subgroups.
Supplementary Information
Below is the link to the electronic supplementary material.
Acknowledgements
Funding
No funding or sponsorship was received for this study or publication of this article.
Authorship
All named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this article, take responsibility for the integrity of the work as a whole, and have given their approval for this version to be published.
Authorship Contributions
Study concept was perceived by Noam Tau; study design: Noam Tau, Dafna Yahav; acquisition of data: Noam Tau, interpretation of data: Noam Tau, Dafna Yahav, Daniel Shepshelovich, drafting of the manuscript: Noam Tau, Dafna Yahav; critical revision of the manuscript: all authors.
Disclosures
Dafna Yahav, Daniel Shepshelovich and Noam Tau have nothing to disclose.
Compliance with Ethics Guidelines
Ethical approval was not required for this study, as data were collected from public databases.
Data Availability
Data sharing is not applicable to this article as no datasets were generated or analyzed during the current stud other than the data provided in Table 1.
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Associated Data
This section collects any data citations, data availability statements, or supplementary materials included in this article.
Supplementary Materials
Data Availability Statement
Data sharing is not applicable to this article as no datasets were generated or analyzed during the current stud other than the data provided in Table 1.