论文信息 - PEGylation does not significantly change the initial intravenous or subcutaneous pharmacokinetics or lymphatic exposure of trastuzumab in rats but increases plasma clearance after subcutaneous administration.

PEGylation does not significantly change the initial intravenous or subcutaneous pharmacokinetics or lymphatic exposure of trastuzumab in rats but increases plasma clearance after subcutaneous administration.

The lymphatic system plays a major role in the metastatic dissemination of cancer and has an integral role in immunity. PEGylation enhances drainage and lymphatic uptake following subcutaneous (sc) administration of proteins and protein-like polymers, but the impact of PEGylation of very large proteins (such as antibodies) on subcutaneous and lymphatic pharmacokinetics is unknown. This study therefore aimed to evaluate the impact of PEGylation on the sc absorption and lymphatic disposition of the anti-HER2 antibody trastuzumab in rats. PEG-trastuzumab was generated via the conjugation of a single 40 kDa PEG-NHS ester to trastuzumab. PEG-trastuzumab showed a 5-fold reduction in HER2 binding affinity, however the in vitro growth inhibitory effects were preserved as a result of changes in cellular trafficking when compared to native trastuzumab. The lymphatic pharmacokinetics of PEG-trastuzumab was evaluated in thoracic lymph duct cannulated rats after iv and sc administration and compared to the pharmacokinetics of native trastuzumab. The iv pharmacokinetics and lymphatic exposure of PEG-trastuzumab was similar when compared to trastuzumab. After sc administration, initial plasma pharmacokinetics and lymphatic exposure were also similar between PEG-trastuzumab and trastuzumab, but the absolute bioavailability of PEG-trastuzumab was 100% when compared to 86.1% bioavailability for trastuzumab. In contrast to trastuzumab, PEG-trastuzumab showed accelerated plasma clearance beginning approximately 7 days after sc, but not iv, administration, presumably as a result of the generation of anti-PEG IgM. This work suggests that PEGylation does not significantly alter the lymphatic disposition of very large proteins, and further suggests that it is unlikely to benefit therapy with monoclonal antibodies.

[1] France Mentré,et al. Metrics for External Model Evaluation with an Application to the Population Pharmacokinetics of Gliclazide , 2006, Pharmaceutical Research.

[2] J. Moffat,et al. Targeting HER2+ breast cancer cells: lysosomal accumulation of anti-HER2 antibodies is influenced by antibody binding site and conjugation to polymeric nanoparticles. , 2013, Journal of controlled release : official journal of the Controlled Release Society.

[3] D. Owen,et al. Methotrexate-conjugated PEGylated dendrimers show differential patterns of deposition and activity in tumor-burdened lymph nodes after intravenous and subcutaneous administration in rats. , 2015, Molecular pharmaceutics.

[4] Jerome Wielens,et al. Potent hepatitis C inhibitors bind directly to NS5A and reduce its affinity for RNA , 2014, Scientific Reports.

[5] G. Edwards,et al. Lymphatic transport of proteins after s.c. injection: implications of animal model selection. , 2001, Advanced drug delivery reviews.

[6] C. Hudis. Trastuzumab--mechanism of action and use in clinical practice. , 2007, The New England journal of medicine.

[7] L. Old,et al. Pharmacokinetics and microdistribution of polyethylene glycol‐modified humanized A33 antibody targeting colon cancer xenografts , 2000, International journal of cancer.

[8] Hideyoshi Harashima,et al. A multifunctional envelope type nano device (MEND) for gene delivery to tumours based on the EPR effect: a strategy for overcoming the PEG dilemma. , 2011, Advanced drug delivery reviews.

[9] D. Owen,et al. Capping methotrexate α-carboxyl groups enhances systemic exposure and retains the cytotoxicity of drug conjugated PEGylated polylysine dendrimers. , 2011, Molecular pharmaceutics.

[10] S. Chandarlapaty,et al. HER2-amplified breast cancer: mechanisms of trastuzumab resistance and novel targeted therapies , 2011, Expert review of anticancer therapy.

[11] Steven W. Martin,et al. Lymphatic Absorption Is the Primary Contributor to the Systemic Availability of Epoetin Alfa following Subcutaneous Administration to Sheep , 2005, Journal of Pharmacology and Experimental Therapeutics.

[12] T. Berg,et al. Uptake, intracellular transport, and degradation of polyethylene glycol-modified asialofetuin in hepatocytes. , 1992, The Journal of biological chemistry.

[13] U. Holzgrabe,et al. Systematic Comparison of the Population Pharmacokinetics and Pharmacodynamics of Piperacillin in Cystic Fibrosis Patients and Healthy Volunteers , 2007, Antimicrobial Agents and Chemotherapy.

[14] Girardet Re,et al. Long term physiologic study of thoracic duct lymph and lymphocytes in rat and man. , 1977 .

[15] L Cohen,et al. Physical and psychological morbidity after axillary lymph node dissection for breast cancer. , 1999, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[16] Jurgen Bernd Bulitta,et al. Development of a New Pre- and Post-Processing Tool (SADAPT-TRAN) for Nonlinear Mixed-Effects Modeling in S-ADAPT , 2011, The AAPS Journal.

[17] I. Madshus,et al. Herceptin‐induced inhibition of ErbB2 signaling involves reduced phosphorylation of Akt but not endocytic down‐regulation of ErbB2 , 2005, International journal of cancer.

[18] S. Banerjee,et al. Poly(ethylene glycol)-Prodrug Conjugates: Concept, Design, and Applications , 2012, Journal of drug delivery.

[19] S. Akilesh,et al. FcRn: the neonatal Fc receptor comes of age , 2007, Nature Reviews Immunology.

[20] R. Ling,et al. Drug concentrations in axillary lymph nodes after lymphatic chemotherapy on patients with breast cancer , 2004, Breast Cancer Research.

[21] Y. Vugmeyster,et al. Pharmacokinetics and toxicology of therapeutic proteins: Advances and challenges. , 2012, World journal of biological chemistry.

[22] Christopher J H Porter,et al. PEGylated polylysine dendrimers increase lymphatic exposure to doxorubicin when compared to PEGylated liposomal and solution formulations of doxorubicin. , 2013, Journal of controlled release : official journal of the Controlled Release Society.

[23] C. Perry,et al. Spotlight on Trastuzumab in Metastatic Breast Cancer Overexpressing HER2 , 2002 .

[24] M. R. Sherman,et al. Role of the Methoxy Group in Immune Responses to mPEG-Protein Conjugates , 2012, Bioconjugate chemistry.

[25] F. Montemurro,et al. Trastuzumab: mechanism of action, resistance and future perspectives in HER2-overexpressing breast cancer. , 2007, Annals of oncology : official journal of the European Society for Medical Oncology.

[26] E. Fiebiger,et al. The Immunologic Functions of the Neonatal Fc Receptor for IgG , 2012, Journal of Clinical Immunology.

[27] Marc Buyse,et al. Adjuvant trastuzumab in HER2-positive breast cancer. , 2011, The New England journal of medicine.

[28] M. Swartz,et al. The physiology of the lymphatic system. , 2001, Advanced drug delivery reviews.

[29] G. Edwards,et al. Systemic availability and lymphatic transport of human growth hormone administered by subcutaneous injection. , 2000, Journal of pharmaceutical sciences.

[30] Leonid Kagan,et al. Pharmacokinetic Modeling of the Subcutaneous Absorption of Therapeutic Proteins , 2014, Drug Metabolism and Disposition.

[31] Y. Hayashi,et al. Membrane protein molecular weight determined by low-angle laser light-scattering photometry coupled with high-performance gel chromatography. , 1989, Methods in enzymology.

[32] G. Storm,et al. Liposomes to target the lymphatics by subcutaneous administration. , 2001, Advanced drug delivery reviews.

[33] A. Supersaxo,et al. Effect of Molecular Weight on the Lymphatic Absorption of Water-Soluble Compounds Following Subcutaneous Administration , 1990, Pharmaceutical Research.

[34] S. Prabhu,et al. Pharmacokinetics, metabolism and distribution of PEGs and PEGylated proteins: quo vadis? , 2014, Drug discovery today.

[35] C. Jackisch,et al. Subcutaneous administration of rituximab (MabThera) and trastuzumab (Herceptin) using hyaluronidase , 2013, British Journal of Cancer.

[36] Steven W. Martin,et al. Pharmacokinetic Model to Describe the Lymphatic Absorption of r-metHu-Leptin After Subcutaneous Injection to Sheep , 2003, Pharmaceutical Research.

[37] L. Kaminskas,et al. Differences in colloidal structure of PEGylated nanomaterials dictate the likelihood of accelerated blood clearance. , 2011, Journal of pharmaceutical sciences.

[38] C. Porter,et al. Subcutaneous drug delivery and the role of the lymphatics. , 2005, Drug discovery today. Technologies.

[39] Daniela Bumbaca,et al. Physiochemical and Biochemical Factors Influencing the Pharmacokinetics of Antibody Therapeutics , 2012, The AAPS Journal.

[40] L. Kaminskas,et al. PEGylation of polylysine dendrimers improves absorption and lymphatic targeting following SC administration in rats. , 2009, Journal of controlled release : official journal of the Controlled Release Society.

[41] G. Edwards,et al. Lymphatic Absorption Is a Significant Contributor to the Subcutaneous Bioavailability of Insulin in a Sheep Model , 2001, Pharmaceutical Research.

[42] M. Skobe,et al. Lymphatic function, lymphangiogenesis, and cancer metastasis , 2001, Microscopy research and technique.

[43] C. Porter,et al. Lymphatic transport of proteins after subcutaneous administration. , 2000, Journal of pharmaceutical sciences.

[44] A E Giuliano,et al. Sentinel lymphadenectomy in breast cancer. , 1997, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[45] J. Reichert,et al. Development trends for human monoclonal antibody therapeutics , 2010, Nature Reviews Drug Discovery.

[46] D. Levêque. Subcutaneous administration of anticancer agents. , 2014, Anticancer research.

[47] F. Veronese. Peptide and protein PEGylation: a review of problems and solutions. , 2001, Biomaterials.

[48] M. R. Sherman,et al. Selectivity of binding of PEGs and PEG-like oligomers to anti-PEG antibodies induced by methoxyPEG-proteins. , 2014, Molecular Immunology.

[49] G. Edwards,et al. Lymphatic Absorption of Subcutaneously Administered Proteins: Influence of Different Injection Sites on the Absorption of Darbepoetin Alfa Using a Sheep Model , 2007, Drug Metabolism and Disposition.

[50] M Jamei,et al. Incorporating Target Shedding Into a Minimal PBPK–TMDD Model for Monoclonal Antibodies , 2014, CPT: pharmacometrics & systems pharmacology.

[51] U. Schubert,et al. Poly(ethylene glycol) in Drug Delivery: Pros and Cons as Well as Potential Alternatives. , 2011 .

[52] Xi Zhan,et al. Effect of the poly(ethylene glycol) (PEG) density on the access and uptake of particles by antigen-presenting cells (APCs) after subcutaneous administration. , 2012, Molecular pharmaceutics.

[53] C. Porter,et al. The lymphatic system plays a major role in the intravenous and subcutaneous pharmacokinetics of trastuzumab in rats. , 2014, Molecular pharmaceutics.

[54] W. Lencer,et al. The recycling and transcytotic pathways for IgG transport by FcRn are distinct and display an inherent polarity , 2009, The Journal of cell biology.

[55] Ben J Boyd,et al. Cationic poly-L-lysine dendrimers: pharmacokinetics, biodistribution, and evidence for metabolism and bioresorption after intravenous administration to rats. , 2006, Molecular pharmaceutics.

[56] Christopher J H Porter,et al. PEGylation of interferon α2 improves lymphatic exposure after subcutaneous and intravenous administration and improves antitumour efficacy against lymphatic breast cancer metastases. , 2013, Journal of controlled release : official journal of the Controlled Release Society.