Presentations include new analysis from the PATH trial, the largest clinical trial in CIDP
| KING OF PRUSSIA, Pa., July 20, 2018 /PRNewswire/ -- Global biotherapeutics leader CSL Behring today announced that it will support the presentation of 14 scientific posters at the 2018 annual meeting of the Peripheral Nerve Society (PNS). Most notably, neuromuscular medical research from the PATH (Polyneuropathy and Treatment with Hizentra) study, the largest ever Chronic Inflammatory Demyelinating Polyneuropathy (CIDP) trial, will be highlighted and new data will be presented for the first time. In addition, CSL Behring will host a symposium, “Managing CIDP with Immunoglobulin: A Clinician’s Guide”. “The PATH extension study data being presented at PNS highlights our commitment to continuing CIDP research and our promise to deliver innovations that clinicians can use,” said Debra Bensen-Kennedy, MD, Vice President for Medical Affairs, North America, CSL Behring. “For that reason, our symposium focuses on providing health care professionals with real world, practical information on CIDP treatment and response measurement, providing them with tools to deliver new options to their patients.” Sunday’s Symposium, “Managing CIDP with Immunoglobulin: A Clinician’s guide” (July 22, 6 p.m. EST) will be chaired by Richard A. Lewis (professor of neurology, Cedars Sinai Medical Center, Los Angeles) and will feature a lecture on “Subcutaneous Immunoglobulin in CIDP: The Evidence” by Thomas Harbo (neurologist, Aarhus University Hospital, Aarhus, Denmark), a review of “Practical Aspects in Subcutaneous Immunoglobulin Administration” by Melody Bullock (registered nurse and infusion science specialist, CSL Behring) and a review from Jeffrey A. Allen (neurologist, University of Minnesota, Minneapolis) on “Objectives Measures You Should Use to Monitor CIDP and Treatment Response.” About CIDP About Hizentra® Important Safety Information for the U.S.
For subcutaneous infusion only.
Hizentra is contraindicated in patients with a history of anaphylactic or severe systemic reaction to human immune globulin (Ig) or components of Hizentra (eg, polysorbate 80), as well as in patients with immunoglobulin A deficiency with antibodies against IgA and a history of hypersensitivity. Because Hizentra contains L-proline as stabilizer, use in patients with hyperprolinemia is contraindicated. IgA-deficient patients with anti-IgA antibodies are at greater risk of severe hypersensitivity and anaphylactic reactions. Thrombosis may occur following treatment with Ig products, including Hizentra. Monitor patients for aseptic meningitis syndrome (AMS), which may occur following treatment with Ig products, including Hizentra. In patients at risk of acute renal failure, monitor renal function, including blood urea nitrogen, serum creatinine and urine output. In addition, monitor patients for clinical signs of hemolysis or pulmonary adverse reactions (eg, transfusion-related acute lung injury [TRALI]). Hizentra is derived from human blood. The risk of transmission of infectious agents, including viruses and, theoretically, the Creutzfeldt-Jakob disease (CJD) agent and its variant (vCJD), cannot be completely eliminated. The most common adverse reactions (observed in ≥5% of study subjects) were local infusion-site reactions, as well as headache, diarrhea, fatigue, back pain, nausea, extremity pain, cough, upper respiratory tract infection, rash, pruritus, vomiting, upper abdominal pain, migraine, arthralgia, pain, fall, and nasopharyngitis. The passive transfer of antibodies can interfere with response to live virus vaccines and lead to misinterpretation of serologic test results. Full Hizentra prescribing information can be found at http://labeling.cslbehring.com/PI/US/Hizentra/EN/Hizentra-Prescribing-Information.pdf. About Privigen® Important Safety Information for the U.S.
WARNING: THROMBOSIS, RENAL DYSFUNCTION AND ACUTE RENAL FAILURE
See full prescribing information for complete boxed warning. In patients at risk of developing acute renal failure, monitor urine output and renal function, including blood urea nitrogen and serum creatinine. Hyperproteinemia, increased serum viscosity, or hyponatremia can occur with Privigen. Infrequently, aseptic meningitis syndrome (AMS) may occur--especially with high doses or rapid infusion. Hemolysis, either intravascular or due to enhanced red blood cell sequestration, may occur. Risk factors include non-O blood group and high doses. Closely monitor patients for hemolysis and hemolytic anemia. During and shortly following Privigen infusion, elevations of systolic and diastolic blood pressure (including cases of hypertensive urgency) have been observed. These elevations resolved or significantly improved within hours with oral anti-hypertensive therapy or observation alone. Check patients for a history of hypertension and monitor blood pressure during this period. Consider relative risks and benefits before prescribing high-dose regimen for chronic ITP and CIDP in patients at increased risk of thrombosis, hemolysis, acute kidney injury or volume overload. Monitor patients for pulmonary adverse reactions (transfusion-related acute lung injury [TRALI]). Privigen is derived from human plasma. The risk of transmission of infectious agents, including viruses and, theoretically, the Creutzfeldt-Jakob disease (CJD) agent and its variant (vCJD), cannot be completely eliminated. In clinical studies of patients with PI, the most common adverse reactions to Privigen, observed in >5% of subjects, were headache, fatigue, nausea, chills, vomiting, back pain, pain, elevated body temperature, abdominal pain, diarrhea, cough, stomach discomfort, chest pain, joint swelling/effusion, influenza-like illness, pharyngolaryngeal pain, urticaria, and dizziness. Serious adverse reactions were hypersensitivity, chills, fatigue, dizziness, and increased body temperature. In clinical studies of patients being treated for chronic ITP, the most common adverse reactions, seen in >5% of subjects, were laboratory findings consistent with hemolysis, headache, elevated body temperature, anemia, nausea, and vomiting. A serious adverse reaction was aseptic meningitis syndrome. In clinical studies of patients being treated for CIDP, the most common reactions, observed in >5% of subjects, were headache, asthenia, hypertension, nausea, pain in extremity, hemolysis, influenza-like illness, leukopenia, and rash. Serious adverse reactions were hemolysis, exacerbation of CIDP, acute rash, increased diastolic blood pressure, hypersensitivity, pulmonary embolism, respiratory failure, and migraine. Treatment with Privigen might interfere with a patient’s response to live virus vaccines and could lead to misinterpretation of serologic testing. In patients over 65 and those at risk of renal insufficiency, do not exceed recommended dose and infuse at the minimum rate practicable. Full Privigen prescribing information, including the complete boxed warning, can be found at http://www.privigen.com/prescribing-information. About CSL Behring CSL Behring operates one of the world’s largest plasma collection networks, CSL Plasma. The parent company, CSL Limited (ASX: CSL), headquartered in Melbourne, Australia, employs more than 20,000 people, and delivers its life-saving therapies to people in more than 60 countries. For more information visit www.cslbehring.com and follow us on www.Twitter.com/CSLBehring. i Laughlin R.S. et al. Incidence and prevalence of CIDP and the association of diabetes mellitus. Neurology. 7;73(1):39-45. View original content with multimedia:http://www.prnewswire.com/news-releases/csl-behring-hosts-symposium-on-managing-cidp-with-immunoglobulin-supports-14-scientific-posters-and-two-oral-presentations-at-the-2018-peripheral-nerve-society-annual-meeting-300684043.html SOURCE CSL Behring |
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