Effect of a Proposed Trastuzumab Biosimilar Compared With Trastuzumab on Overall Response Rate in Patients With ERBB2 (HER2)–Positive Metastatic Breast Cancer

Rugo, Hope S.; Barve, Abhijit; Waller, Christiane; Hernández-Bronchud, Miguel; Herson, Jay; Yuan, Jiamin; Sharma, Rajiv; Baczkowski, Mark; Kothekar, Mudgal; Loganathan, Subramanian; Manikhas, A.; Bondarenko, Igor; Mukhametshina, Guzel; Nemsadze, Gia; Parra, Joseph D.; Abesamis-Tiambeng, Maria Luisa T.; Baramidze, Kakhaber; Akewanlop, Charuwan; Vynnychenko, I.; Sriuranpong, Virote; Mamillapalli, Gopichand; Ray, Sirshendu; Ruiz, Eduardo Patricio Yanez; Pennella, Eduardo J.

doi:10.1001/jama.2016.18305

Cited by 137 publications

(193 citation statements)

References 20 publications

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“…In 2017, the patent for intravenous trastuzumab (Herceptin) expired across Europe, which stimulated the development of numerous trastuzumab biosimilar agents (Table 1). [1][2][3][4][5] In this issue of the British Journal of Cancer, Lammers et al report evidence establishing another step towards the registration of PF-05280014, a trastuzumab biosimilar candidate developed by Pfizer. 1,[6][7][8] This significant trial has provided clinical efficacy results of this candidate in patients with early breast cancer, and insight into its pharmacokinetic (PK) non-inferiority.…”

Section: Mainmentioning

confidence: 99%

Section: Mainmentioning

confidence: 99%

“…Variable margins of equivalence using different ranges of confidence were prespecified to define equivalence (Table 1). [1][2][3][4][5] This variability reflects the difficulty in reaching a consensus on the acceptable and/or reasonable difference in efficacy of a biosimilar compound.The second parameter of interest to consider is the population studied and the endpoint criterion used to claim equivalence. According to guidelines, clinical trials should be carried out on a sensitive and homogenous patient population, using endpoints that will; most easily detect differences between the biosimilar and the reference product.…”

mentioning

confidence: 99%

“…20 If a hierarchy based on clinical assessment could be developed for trastuzumab biosimilar candidates, then the agents with a favourable clinical assessment using pCR after neoadjuvant therapy might appear at the top of such classification (Table 1). [1][2][3][4][5] A single clinical study, in either the metastatic or the neoadjuvant setting, is usually sufficient to prove the equivalent efficacy of a biosimilar drug. CPT-6 was previously assessed in studies using both settings, but this was due to small changes in the production process that required duplication of all the comparability exercises .…”

mentioning

confidence: 99%

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Can we establish a hierarchy among trastuzumab biosimilar candidates?

Pivot¹,

Petit²

2018

Br J Cancer

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The European patent for intravenous trastuzumab lapsed in 2017, and this stimulated research into a number of trastuzumab biosimilars. Quality assessment of their development and clinical results might enable establishment of a clinical hierarchy of these agents. This editorial will underline the key points for consideration when determining such an evaluation.British Journal of Cancer (2018) 119:263-265; https://doi.org/10.1038/s41416-018-0171-1 MAINThe extraordinary clinical achievements of trastuzumab have made history in the systemic management of breast cancer. Unfortunately, it is not uniformly available for routine use owing to its prohibitively high cost. With financial contingencies following the economic crisis together with rapidly increasing healthcare costs, even the richest countries are exploring ways to reduce their healthcare expenditures. In 2017, the patent for intravenous trastuzumab (Herceptin) expired across Europe, which stimulated the development of numerous trastuzumab biosimilar agents (Table 1). [1][2][3][4][5] In this issue of the British Journal of Cancer, Lammers et al. report evidence establishing another step towards the registration of PF-05280014, a trastuzumab biosimilar candidate developed by Pfizer. 1,[6][7][8] This significant trial has provided clinical efficacy results of this candidate in patients with early breast cancer, and insight into its pharmacokinetic (PK) non-inferiority.The development of a biosimilar drug requires the collation of extensive pre-clinical comparability studies to demonstrate similar structural, physicochemical, and functional biological characteristics with the referent medical product. 9,10 . PK comparability in animal models is required prior to the first in-human study, and this is usually aimed at demonstrating PK equivalence between the biosimilar candidate and the referent. These steps have already been successfully achieved for PF-05280014.6,7 Treatment with trastuzumab can result in the production of anti-trastuzumab antibodies; therefore, initial phase I trials for PK assessment include healthy male subjects, because they are less likely to require treatment with trastuzumab for breast cancer in the future. Notably, several previous studies have validated the absence of observable discrepancies in PK profiles for trastuzumab between healthy volunteers and patients. 2,4,11,12 Iterative drug administration causes an accumulation of plasma drug levels, thus resulting in an increase of the average AUC (0-t) . For trastuzumab exposure, large variability in the AUC (0-t) is observed up to cycle 5, beyond which the values become stable and homogeneous over time. 13,14 Therefore, a large randomised study aimed at comparing the activities should also perform a PK assessment in patients receiving iterative administration.A randomised clinical study represents the ultimate step in the path towards drug registration, with the intention of providing evidence for similar efficacy between the biosimilar candidate and the reference medical product in a...

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Section: Mainmentioning

confidence: 99%

Section: Mainmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Can we establish a hierarchy among trastuzumab biosimilar candidates?

Pivot¹,

Petit²

2018

Br J Cancer

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“…106 In December 2017, MYL-1401O became the first trastuzumab biosimilar to be licensed by the US FDA, as trastuzumab-dkst 107 ; the evidence supporting biosimilarity included a comparative study carried out in the metastatic breast cancer setting. 108 Later that month, MYL-1401O was approved in Brazil, where it will be commercialized by local pharmaceutical company Libbs Farmaceutica. 109 Although the product will initially be supplied to Libbs by the manufacturer Biocon, over time the technology will be transferred to Libbs and public partner Butantan, enabling domestic production.…”

Section: Biosimilar Monoclonal Antibody Therapies Relevant To Oncologmentioning

confidence: 99%

Biosimilars in oncology and inflammatory diseases: current and future considerations for clinicians in Latin America

Scheinberg

Pineda

Castañeda‐Hernández

et al. 2018

mAbs

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Biological therapies have revolutionized the treatment of several cancers and systemic immune-mediated inflammatory conditions. Expiry of patents protecting a number of biologics has provided the opportunity to commercialize highly similar versions, known as biosimilars. Biosimilars are approved by regulatory agencies via an independent pathway that requires extensive head-to-head comparison with the originator product. Biosimilars have the potential to provide savings to healthcare systems and expand patient access to biologics. In Latin American countries, regulatory frameworks for biosimilar approval have been introduced in recent years, and biosimilars of monoclonal antibody and fusion protein therapies are now emerging. However, the situation in this region is complicated by the presence of “non-comparable biotherapeutics” (also known as “intended copies”), which have not been rigorously compared with the originator product. We review the considerations for clinicians in Latin American countries, focusing on monoclonal antibody biosimilars relevant to oncology, rheumatology, gastroenterology, and dermatology.

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Scientific Evidence and Financial Obligations to Ensure Access to Biosimilars for Cancer Treatment

Bauchner¹,

Fontanarosa²,

Golub³

2017

JAMA

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Articles in medical journals add to the scientific body of research that ultimately influences care. On rare occasions a single study changes the practice of medicine, but in general most clinical research reports contribute to a body of evidence that becomes part of the fabric of clinical decision making, including individual decisions of physicians and patients as well as use in guidelines and recommendations of professional societies and governmental agencies.In this issue of JAMA, Rugo and colleagues 1 report findings from a multicenter clinical trial that may influence care for patients with breast cancer around the world. The authors evaluated the equivalence of a proposed trastuzumab biosimilar compared with the standard therapy, the humanized monoclonal antibody trastuzumab, for achieving overall response and for safety among 458 women without prior treatment for ERBB2 (HER2)-positive metastatic breast cancer.The overall response rate (ie, complete or partial clinical response) at 24 weeks for the proposed biosimilar plus a taxane was 69.6% (95% CI, 63.62% to 75.51%) compared with 64.0% (95% CI, 57.81% to 70.26%) for trastuzumab plus a taxane. The overall response rate ratio (1.09 [90% CI, 0.97 to 1.21]) and overall response rate difference (5.53 [95% CI, −3.08 to 14.04]) met predefined criteria for equivalence. The rates of adverse events were similar in the 2 treatment groups. The results of this investigation are promising, but as the authors rightfully acknowledge, further research is needed to assess safety as well as long-term clinical outcomes.Trastuzumab combined with chemotherapy has improved survival for patients with ERBB2-positive metastatic breast cancer. However, because of its high cost (approximately $64 000 for treatment over 1 year), 2 trastuzumab is not widely available for patients in some countries. The availability of a biosimilar agent that achieves equivalent clinical outcomes at lower cost could enable many patients with breast cancer to have access to a therapy that may improve survival. Moreover, given the large number of patients with breast cancer, widespread use of this trastuzumab biosimilar evaluated by Rugo et al (if approved for use by the US Food and Drug Administration [FDA], the European Medicines Agency, and other regulatory agencies) also could have financial implications for the manufacturer of this product.

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Effect of a Proposed Trastuzumab Biosimilar Compared With Trastuzumab on Overall Response Rate in Patients With ERBB2 (HER2)–Positive Metastatic Breast Cancer

Cited by 137 publications

References 20 publications

Can we establish a hierarchy among trastuzumab biosimilar candidates?

Can we establish a hierarchy among trastuzumab biosimilar candidates?

Biosimilars in oncology and inflammatory diseases: current and future considerations for clinicians in Latin America

Scientific Evidence and Financial Obligations to Ensure Access to Biosimilars for Cancer Treatment

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