{"id":55070,"date":"2023-03-22T11:05:24","date_gmt":"2023-03-22T10:05:24","guid":{"rendered":"https:\/\/pharma-trend.com\/en\/alzheon-to-present-biomarker-brain-preservation-and-clinical-effects-of-oral-tablet-alz-801-valiltramiprosate-at-upcoming-ad-pd-2023-conference-in-gothenburg-sweden\/"},"modified":"2023-03-22T11:05:24","modified_gmt":"2023-03-22T10:05:24","slug":"alzheon-to-present-biomarker-brain-preservation-and-clinical-effects-of-oral-tablet-alz-801-valiltramiprosate-at-upcoming-ad-pd-2023-conference-in-gothenburg-sweden","status":"publish","type":"post","link":"https:\/\/pharma-trend.com\/en\/alzheon-to-present-biomarker-brain-preservation-and-clinical-effects-of-oral-tablet-alz-801-valiltramiprosate-at-upcoming-ad-pd-2023-conference-in-gothenburg-sweden\/","title":{"rendered":"Alzheon to Present Biomarker, Brain Preservation and Clinical Effects of Oral Tablet ALZ-801 (Valiltramiprosate) at Upcoming AD\/PD 2023 Conference in Gothenburg, Sweden"},"content":{"rendered":"<div>\n<p class=\"bwalignc\">\n<i>Industry-Leading Results Position ALZ-801 to Potentially Become the First Oral Agent that Can Slow or Even Stop and Prevent Alzheimer\u2019s Pathology in Patients and Healthy Individuals at Risk for the Disease<\/i>\n<\/p>\n<p class=\"bwalignc\">\n<i>Robust Disease-Modifying Effects Observed Through 52 Weeks of Treatment with ALZ-801 Tablet in APOE4 Carriers with Early Alzheimer\u2019s Disease<\/i>\n<\/p>\n<p class=\"bwalignc\">\n<i>New Data Further Validate Alzheon Science and Unique Mechanism of Action of Oral ALZ-801 as Potentially First and Only Amyloid Oligomer Prevention Therapy<\/i>\n<\/p>\n<p class=\"bwalignc\">\n<i>Advances in Development of Proprietary Assay for Detection of A<\/i><i>\u03b2<\/i><i>(1-42) Oligomers Aligns Novel Diagnostic with ALZ-801 Commercial Launch in 2025<\/i>\n<\/p>\n<p class=\"bwalignc\">\n<i>Safety Profile in ALZ-801 Studies Remains Favorable &amp; Consistent with Prior Data in Over 2,800 Alzheimer&#8217;s Patients, with no Increased Risk of Vasogenic Brain Edema<\/i>\n<\/p>\n<p>FRAMINGHAM, Mass.&#8211;(BUSINESS WIRE)&#8211;<a href=\"https:\/\/twitter.com\/hashtag\/ALZ801?src=hash\" target=\"_blank\" rel=\"noopener\">#ALZ801<\/a>&#8212;<a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=http%3A%2F%2Fwww.alzheon.com%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Alzheon%2C+Inc.&amp;index=1&amp;md5=ec2922dd47edad84acd8dde76d474f08\" rel=\"nofollow noopener\" shape=\"rect\">Alzheon, Inc.<\/a>, a clinical-stage biopharmaceutical company developing a broad portfolio of product candidates and diagnostic assays for patients suffering from Alzheimer\u2019s disease (AD) and other neurodegenerative disorders, today announced that it will be presenting interim findings from an ongoing Phase 2 study evaluating ALZ-801 tablet at the upcoming <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fadpd.kenes.com%2F%3Futm_source%3Dgoogle%26utm_medium%3Dsearch%26utm_campaign%3Dregistration%26gclid%3DCj0KCQjwwtWgBhDhARIsAEMcxeCSfVQoz7RSWY7QFd02g0LYcisjEDmk-xJBoJZYqhd7DhM2fX49jX4aAkPvEALw_wcB&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=AD%2FPD+2023+Conference&amp;index=2&amp;md5=bd415d0887facdffabc1a2665c1b909d\" rel=\"nofollow noopener\" shape=\"rect\">AD\/PD 2023 Conference<\/a> to be held from March 28 \u2013 April 1, 2023 in Gothenburg, Sweden.\n<\/p>\n<p><a href=\"https:\/\/mms.businesswire.com\/media\/20230322005010\/en\/1048333\/5\/alzheon_logo-fb.jpg\"><img decoding=\"async\" src=\"https:\/\/mms.businesswire.com\/media\/20230322005010\/en\/1048333\/21\/alzheon_logo-fb.jpg\"><\/a><\/p>\n<p>\n<a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Fpipeline%2Falzheon-alz-801%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=ALZ-801+%28valiltramiprosate%29&amp;index=3&amp;md5=bab0848f7e5f6a4a51e421a545de7083\" rel=\"nofollow noopener\" shape=\"rect\">ALZ-801 (valiltramiprosate)<\/a> is an oral agent in <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fclinicaltrials.gov%2Fct2%2Fshow%2FNCT04770220&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Phase+3+development&amp;index=4&amp;md5=baea6409d5ab55f99a54b153b4f2e8f3\" rel=\"nofollow noopener\" shape=\"rect\">Phase 3 development<\/a> as a potentially disease modifying treatment for AD that blocks formation of neurotoxic soluble beta amyloid (A\u03b2) oligomers causing cognitive decline in Alzheimer\u2019s patients. In mechanism of action studies, ALZ-801 fully inhibited the formation of amyloid oligomers at the Phase 3 clinical dose. ALZ-801 has shown potential for robust efficacy in the highest-risk Alzheimer\u2019s population \u2013 patients with two copies of the apolipoprotein \u03b54 allele (APOE4\/4 homozygotes), and favorable safety with no increased risk of brain vasogenic edema, seen in trials with plaque-clearing antibodies. This population is the focus of Alzheon\u2019s pivotal <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Falzheon-announces-first-patient-dosed-in-apolloe4-phase-3-trial-of-oral-alz-801-in-patients-with-early-alzheimers-disease%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Phase+3+APOLLOE4+trial&amp;index=5&amp;md5=c948c8417ccb9b03555b2e7dbb689fc5\" rel=\"nofollow noopener\" shape=\"rect\">Phase 3 APOLLOE4 trial<\/a> and has the highest likelihood of demonstrating successful efficacy outcomes.\n<\/p>\n<p>\nAlzheon Chief Scientific Officer, John Hey, PhD, will give a podium presentation titled: <i>Significant Biomarker Effects of Oral Anti-Amyloid Agent ALZ-801 (Valiltramiprosate) In Phase 2 Study In APOE4 Carriers With Early Alzheimer\u2019s Disease<\/i>, on March 30, 2023, at 6:50 p.m. CET or 12:50 p.m. EST, as part of the \u201cAD Drug Development Clinical Trials\u201d symposium in Hall C.\n<\/p>\n<p>\nThe open-label Phase 2 trial enrolled subjects at seven sites in the Czech Republic and Netherlands. Study is evaluating effects on plasma biomarkers of AD, hippocampal volume (HV), and clinical outcomes of ALZ-801 265mg BID tablet in Early AD subjects (MMSE 22-30) with APOE4\/4 or APOE3\/4 genotype.\n<\/p>\n<p>\nA total of 84 APOE4 carriers were enrolled and received ALZ-801, with 80 and 75 subjects completing 26 and 52 weeks, respectively. Plasma p-tau<sub>181<\/sub> change from baseline was significant at 13 and 26 weeks and reached -41% at 52 weeks (p=0.016). Bilateral hippocampal volume atrophy at 1 year was reduced by approximately 20% compared to the matched subjects from AD Neuroimaging Initiative. Most common adverse events were mild nausea and COVID infection, with no drug-related serious events and no events of ARIA-E.\n<\/p>\n<p>\n\u201cThe results of this study further confirm both the role of beta amyloid oligomers in the pathobiology of Alzheimer\u2019s disease and the mechanism of action of ALZ-801. By inhibiting the misfolding of amyloid monomers and subsequent formation of neurotoxic amyloid oligomers, we observed a rapid and sustained reduction in plasma p-tau<sub>181<\/sub> as early as 13 weeks, with continued reduction through 52 weeks,\u201d said Dr. Hey. \u201cPreventing oligomer formation with an oral tablet is a simplified approach to disease modification in Alzheimer\u2019s. Phase 2 study results provide compelling evidence for potential efficacy of ALZ-801 in APOE4 carriers with Alzheimer\u2019s disease, who represent two thirds of Alzheimer\u2019s patients. These data also highlight the potential safety and efficacy advantages of ALZ-801 compared to plaque-clearing antibodies, while offering a simplified patient journey towards an effective treatment.\u201d\n<\/p>\n<p>\nAdditionally, poster P0457\/#2737, titled: <i>Utilization of Cyclic Ion Mobility Spectrometry for Detection and Characterization of A<\/i>\u03b2<i>(<\/i><i>1-42) Oligomers<\/i>, highlights progress by the Institute of Organic Chemistry and Biochemistry (IOCB) in collaboration with Alzheon to detect and measure the individual species of beta amyloid oligomers in human CSF. Mikul\u00e1\u0161 Vlk of IOCB will present the poster, with Dr. Hey and other Alzheon scientists among contributing authors.\n<\/p>\n<p>\n\u201cAlzheon has pioneered precision medicine in Alzheimer\u2019s disease by targeting neurotoxic amyloid oligomers, and these promising biomarker, imaging, and clinical data with ALZ-801 provide additional support for our approach. It is becoming apparent that our best opportunity to alter the relentless progression of Alzheimer\u2019s pathology is to identify individuals early in the disease course, ideally before clinical symptoms emerge. Our ability to find these patients is enabled by biomarkers and imaging, and novel detection of neurotoxic oligomers in the initial stages of the amyloid cascade offers potential points of intervention,\u201d said Martin Tolar, MD, PhD, Founder, President, and CEO of Alzheon. \u201cWe are potentially two years from a commercial launch of ALZ-801 in the U.S. and the successful collaboration with IOCB means that we are getting closer to a diagnostic, which would complement our novel therapy, extend the therapeutic window in Alzheimer\u2019s, and further differentiate our treatment approach to this devastating disease.\u201d\n<\/p>\n<p>\n<b>About ALZ-801<br \/>\n<br \/><\/b><a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Fpipeline%2Falzheon-alz-801%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=ALZ-801+%28valiltramiprosate%29&amp;index=6&amp;md5=722dbeac17265f447193d3b3404a60f1\" rel=\"nofollow noopener\" shape=\"rect\">ALZ-801 (valiltramiprosate)<\/a> is an investigational oral agent in <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fclinicaltrials.gov%2Fct2%2Fshow%2FNCT04770220&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Phase+3+development&amp;index=7&amp;md5=776e269a06326de4dcf5f0126de7c563\" rel=\"nofollow noopener\" shape=\"rect\">Phase 3 development<\/a> as a potentially disease modifying treatment for AD.<sup>1,3<\/sup> In mechanism of action studies, ALZ-801 has been shown to fully inhibit the formation of neurotoxic soluble beta amyloid oligomers at the Phase 3 clinical dose.<sup>5,6<\/sup> ALZ\u2011801 acts through a novel <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Famyloid-oligomers%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=enveloping+molecular+mechanism+of+action&amp;index=8&amp;md5=d9d4338054a0e55bed51ad1328b49f5b\" rel=\"nofollow noopener\" shape=\"rect\">enveloping molecular mechanism of action<\/a> to fully block formation of neurotoxic soluble amyloid oligomers in the human brain<sup>7<\/sup> associated with the onset of cognitive symptoms and progression of AD.<sup>1\u20134<\/sup> ALZ-801 received Fast Track designation from the U.S. Food and Drug Administration in 2017. The clinical data for ALZ-801 and Alzheon\u2019s safety database indicate a favorable safety profile.<sup>5\u20137,9<\/sup> The initial <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Fpipeline%2Falzheon-alz-801%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Phase+3+program+for+ALZ-801&amp;index=9&amp;md5=7726b476b6bec8494bf94daf1b7a4829\" rel=\"nofollow noopener\" shape=\"rect\">Phase 3 program for ALZ-801<\/a> is focusing on Early AD patients with the APOE4\/4 genotype, with future expansion to AD treatment and prevention in patients carrying one copy of the APOE4 gene and noncarriers.<sup>1\u20134<\/sup>\n<\/p>\n<p>\n<b>ALZ-801 APOLLOE4 Phase 3 Study<br \/>\n<br \/><\/b>An Efficacy and Safety Study of ALZ-801 in APOE4\/4 Early Alzheimer&#8217;s Disease Subjects (<a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fclinicaltrials.gov%2Fct2%2Fshow%2FNCT04770220&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=NCT04770220&amp;index=10&amp;md5=ab9dc3d59af3f5b3bb731c78fd6bb731\" rel=\"nofollow noopener\" shape=\"rect\">NCT04770220<\/a>): This ongoing study is designed to evaluate the efficacy, safety, biomarker and imaging effects of 265 mg twice daily oral dose of ALZ-801 in Early AD subjects with the APOE4\/4 genotype, who constitute approximately 15% of Alzheimer&#8217;s patients. This is a double-blind, randomized trial comparing oral ALZ-801 to placebo treatment over 78 weeks. The APOLLOE4 trial is supported by a $47 million <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Freporter.nih.gov%2Fproject-details%2F10050013&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=grant+from+the+National+Institute+on+Aging&amp;index=11&amp;md5=77425b019d218ae818f2b3c3e3dfc4f4\" rel=\"nofollow noopener\" shape=\"rect\">grant from the National Institute on Aging<\/a>.\n<\/p>\n<p>\n<b>ALZ-801 Phase 2 Biomarker Study<br \/>\n<br \/><\/b>Biomarker Effects of ALZ-801 in APOE4 Carriers With Early Alzheimer&#8217;s Disease (<a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fclinicaltrials.gov%2Fct2%2Fshow%2FNCT04693520&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=NCT04693520&amp;index=12&amp;md5=56d9499667c3add29323e2bfd4c102d4\" rel=\"nofollow noopener\" shape=\"rect\">NCT04693520<\/a>): This ongoing study is designed to evaluate the effects of 265 mg twice daily oral dose of ALZ-801 on biomarkers of AD pathology in subjects with Early AD, who have either the APOE4\/4 or APOE3\/4 genotype and constitute 65-70% of Alzheimer&#8217;s patients. The study also includes evaluation of clinical efficacy, safety, tolerability, and pharmacokinetic profile of ALZ-801 over 104 weeks of treatment.\n<\/p>\n<p>\n<b>About Alzheon<br \/>\n<br \/><\/b><a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=http%3A%2F%2Fwww.alzheon.com%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Alzheon%2C+Inc.&amp;index=13&amp;md5=d66a862920556b2e3976cd106b5ddba5\" rel=\"nofollow noopener\" shape=\"rect\">Alzheon, Inc.<\/a> is a clinical-stage biopharmaceutical company developing a broad portfolio of product candidates and diagnostic assays for patients suffering from Alzheimer\u2019s disease and other neurodegenerative disorders. We are committed to developing innovative medicines by directly addressing the underlying pathology of neurodegeneration. Our lead Alzheimer\u2019s clinical candidate, <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Fpipeline%2Falzheon-alz-801%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=ALZ-801+%28valiltramiprosate%29&amp;index=14&amp;md5=1af76aa07f70e1301056efad1e43fb67\" rel=\"nofollow noopener\" shape=\"rect\">ALZ-801 (valiltramiprosate)<\/a>, is an oral agent in <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fclinicaltrials.gov%2Fct2%2Fshow%2FNCT04770220&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Phase+3+development&amp;index=15&amp;md5=2c5d364b3f25c0d9a6ba2c34b6d17bdb\" rel=\"nofollow noopener\" shape=\"rect\">Phase 3 development<\/a> as a potentially disease modifying treatment for AD. ALZ-801<sup> <\/sup>is an oral small molecule that fully blocks formation of neurotoxic soluble amyloid oligomers in the brain. Our clinical expertise and technology platform are focused on developing drug candidates and diagnostic assays using a <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzheon.com%2Fclinical-data%2F&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=precision+medicine+approach&amp;index=16&amp;md5=844752c503e20a272f5a48b94c583e0a\" rel=\"nofollow noopener\" shape=\"rect\">precision medicine approach<\/a> based on individual genetic and biomarker information to advance therapies with the greatest impact for patients.\n<\/p>\n<p>\n<b>Alzheon Scientific Publications<br \/>\n<br \/><\/b><sup>1 <\/sup>Tolar M, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Fwww.mdpi.com%2F1422-0067%2F22%2F12%2F6355&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Neurotoxic+Soluble+Amyloid+Oligomers+Drive+Alzheimer%26%238217%3Bs+Pathogenesis+and+Represent+a+Clinically+Validated+Target+for+Slowing+Disease+Progression%2C+International+Journal+of+Molecular+Sciences&amp;index=17&amp;md5=ade9483b7a16b82f7d496f5b9d223926\" rel=\"nofollow noopener\" shape=\"rect\">Neurotoxic Soluble Amyloid Oligomers Drive Alzheimer\u2019s Pathogenesis and Represent a Clinically Validated Target for Slowing Disease Progression, International Journal of Molecular Sciences<\/a>, 2021; 22, 6355.<br \/>\n<br \/><sup>2 <\/sup>Abushakra S, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falz-journals.onlinelibrary.wiley.com%2Fdoi%2F10.1002%2Ftrc2.12117&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=APOE+%26%23949%3B4%2F%26%23949%3B4+Homozygotes+with+Early+Alzheimer%26%238217%3Bs+Disease+Show+Accelerated+Hippocampal+Atrophy+and+Cortical+Thinning+that+Correlates+with+Cognitive+Decline%2C+Alzheimer%26%238217%3Bs+%26amp%3B+Dementia&amp;index=18&amp;md5=66e75ec0812590b46cf310c698853be5\" rel=\"nofollow noopener\" shape=\"rect\">APOE \u03b54\/\u03b54 Homozygotes with Early Alzheimer\u2019s Disease Show Accelerated Hippocampal Atrophy and Cortical Thinning that Correlates with Cognitive Decline, Alzheimer\u2019s &amp; Dementia<\/a>, 2020; 6: e12117.<br \/>\n<br \/><sup>3 <\/sup>Tolar M, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falzres.biomedcentral.com%2Farticles%2F10.1186%2Fs13195-020-00663-w&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Aducanumab%2C+Gantenerumab%2C+BAN2401%2C+and+ALZ-801%26%238212%3Bthe+First+Wave+of+Amyloid-Targeting+Drugs+for+Alzheimer%26%238217%3Bs+Disease+with+Potential+for+Near+Term+Approval%2C+Alzheimer%26%238217%3Bs+Research+%26amp%3B+Therapy%2C&amp;index=19&amp;md5=8272e60771d6cdbde6e5c82a3324e836\" rel=\"nofollow noopener\" shape=\"rect\">Aducanumab, Gantenerumab, BAN2401, and ALZ-801\u2014the First Wave of Amyloid-Targeting Drugs for Alzheimer\u2019s Disease with Potential for Near Term Approval, Alzheimer\u2019s Research &amp; Therapy,<\/a> 2020; 12: 95.<br \/>\n<br \/><sup>4 <\/sup>Tolar M, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Falz-journals.onlinelibrary.wiley.com%2Fdoi%2Ffull%2F10.1016%2Fj.jalz.2019.09.075&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=The+Path+Forward+in+Alzheimer%26%238217%3Bs+Disease+Therapeutics%3A+Reevaluating+the+Amyloid+Cascade+Hypothesis%2C+Alzheimer%26%238217%3Bs+%26amp%3B+Dementia%2C&amp;index=20&amp;md5=51daaf147c57ae970091c8782ae9ce04\" rel=\"nofollow noopener\" shape=\"rect\">The Path Forward in Alzheimer\u2019s Disease Therapeutics: Reevaluating the Amyloid Cascade Hypothesis, Alzheimer\u2019s &amp; Dementia,<\/a> 2019; 1-8.<br \/>\n<br \/><sup>5 <\/sup>Hey JA, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Flink.springer.com%2Farticle%2F10.1007%2Fs40263-018-0554-0&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Discovery+and+Identification+of+an+Endogenous+Metabolite+of+Tramiprosate+and+Its+Prodrug+ALZ-801+that+Inhibits+Beta+Amyloid+Oligomer+Formation+in+the+Human+Brain%2C+CNS+Drugs%2C&amp;index=21&amp;md5=0129b6fc8b40ee8e8c85c6b247a6661e\" rel=\"nofollow noopener\" shape=\"rect\">Discovery and Identification of an Endogenous Metabolite of Tramiprosate and Its Prodrug ALZ-801 that Inhibits Beta Amyloid Oligomer Formation in the Human Brain, CNS Drugs,<\/a> 2018; 32(9): 849-861.<br \/>\n<br \/><sup>6 <\/sup>Hey JA, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Flink.springer.com%2Farticle%2F10.1007%2Fs40262-017-0608-3&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Clinical+Pharmacokinetics+and+Safety+of+ALZ-801%2C+a+Novel+Prodrug+of+Tramiprosate+in+Development+for+the+Treatment+of+Alzheimer%26%238217%3Bs+Disease%2C+Clinical+Pharmacokinetics%2C&amp;index=22&amp;md5=d58f9e5c9dd359a911fb6d082084f7f7\" rel=\"nofollow noopener\" shape=\"rect\">Clinical Pharmacokinetics and Safety of ALZ-801, a Novel Prodrug of Tramiprosate in Development for the Treatment of Alzheimer\u2019s Disease, Clinical Pharmacokinetics,<\/a> 2018; 57(3): 315\u2013333.<br \/>\n<br \/><sup>7 <\/sup>Abushakra S, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=http%3A%2F%2Fwww.jpreventionalzheimer.com%2Fall-issues.html%3Farticle%3D328&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Clinical+Effects+of+Tramiprosate+in+APOE4%2F4+Homozygous+Patients+with+Mild+Alzheimer%26%238217%3Bs+Disease+Suggest+Disease+Modification+Potential%2C+Journal+of+Prevention+of+Alzheimer%26%238217%3Bs+Disease%2C&amp;index=23&amp;md5=92de6154ee36d41b49b28aa628d3ab99\" rel=\"nofollow noopener\" shape=\"rect\">Clinical Effects of Tramiprosate in APOE4\/4 Homozygous Patients with Mild Alzheimer\u2019s Disease Suggest Disease Modification Potential, Journal of Prevention of Alzheimer\u2019s Disease,<\/a> 2017; 4(3): 149-156.<br \/>\n<br \/><sup>8 <\/sup>Kocis P, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=https%3A%2F%2Flink.springer.com%2Farticle%2F10.1007%2Fs40263-017-0434-z&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Elucidating+the+A%26%23946%3B42+Anti-Aggregation+Mechanism+of+Action+of+Tramiprosate+in+Alzheimer%26%238217%3Bs+Disease%3A+Integrating+Molecular+Analytical+Methods%2C+Pharmacokinetic+and+Clinical+Data%2C+CNS+Drugs%2C&amp;index=24&amp;md5=53fc073a081e35122dee87ed2717a01c\" rel=\"nofollow noopener\" shape=\"rect\">Elucidating the A\u03b242 Anti-Aggregation Mechanism of Action of Tramiprosate in Alzheimer\u2019s Disease: Integrating Molecular Analytical Methods, Pharmacokinetic and Clinical Data, CNS Drugs,<\/a> 2017; 31(6): 495-509.<br \/>\n<br \/><sup>9 <\/sup>Abushakra S, et al: <a target=\"_blank\" href=\"https:\/\/cts.businesswire.com\/ct\/CT?id=smartlink&amp;url=http%3A%2F%2Fwww.jpreventionalzheimer.com%2Fall-issues.html%3Farticle%3D240&amp;esheet=53364326&amp;newsitemid=20230322005010&amp;lan=en-US&amp;anchor=Clinical+Benefits+of+Tramiprosate+in+Alzheimer%26%238217%3Bs+Disease+Are+Associated+with+Higher+Number+of+APOE4+Alleles%3A+The+%26%238220%3BAPOE4+Gene-Dose+Effect%2C%26%238221%3B+Journal+of+Prevention+of+Alzheimer%26%238217%3Bs+Disease%2C&amp;index=25&amp;md5=c8881659cc174b06678f8342941afe8d\" rel=\"nofollow noopener\" shape=\"rect\">Clinical Benefits of Tramiprosate in Alzheimer\u2019s Disease Are Associated with Higher Number of APOE4 Alleles: The \u201cAPOE4 Gene-Dose Effect,\u201d Journal of Prevention of Alzheimer\u2019s Disease,<\/a> 2016; 3(4): 219-228.\n<\/p>\n<p> <b>Contacts<\/b> <\/p>\n<p>\n<b>Media<\/b><br \/>Adem Albayrak<br \/>\n<br \/>Alzheon, Inc.<br \/>\n<br \/>508.861.7709<br \/>\n<br \/><a target=\"_blank\" href=\"&#x6d;&#x61;&#x69;&#x6c;&#x74;&#x6f;&#x3a;&#x61;&#100;&#101;&#109;&#46;&#97;&#108;&#98;ayra&#x6b;&#x40;&#x61;&#x6c;&#x7a;&#x68;&#x65;&#x6f;&#x6e;&#46;&#99;&#111;&#109;\" rel=\"nofollow noopener\" shape=\"rect\">&#97;d&#x65;m&#x2e;&#97;&#x6c;&#98;&#x61;&#121;r&#x61;k&#x40;&#97;&#x6c;&#122;&#x68;&#101;&#x6f;&#110;&#46;&#x63;o&#x6d;<\/a>\n<\/p>\n<\/div>\n","protected":false},"excerpt":{"rendered":"<p>Industry-Leading Results Position ALZ-801 to Potentially Become the First Oral Agent that Can Slow or Even Stop and Prevent Alzheimer\u2019s Pathology in Patients and Healthy Individuals at Risk for the Disease Robust Disease-Modifying Effects Observed Through 52 Weeks of Treatment with ALZ-801 Tablet in APOE4 Carriers with Early Alzheimer\u2019s Disease New Data Further Validate Alzheon &#8230; <span class=\"more\"><a class=\"more-link\" href=\"https:\/\/pharma-trend.com\/en\/alzheon-to-present-biomarker-brain-preservation-and-clinical-effects-of-oral-tablet-alz-801-valiltramiprosate-at-upcoming-ad-pd-2023-conference-in-gothenburg-sweden\/\">[Read more&#8230;]<\/a><\/span><\/p>\n","protected":false},"author":4,"featured_media":0,"comment_status":"closed","ping_status":"closed","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[13],"tags":[],"class_list":{"0":"entry","1":"post","2":"publish","3":"author-business","4":"post-55070","6":"format-standard","7":"category-industry"},"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.4 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>Alzheon to Present Biomarker, Brain Preservation and Clinical Effects of Oral Tablet ALZ-801 (Valiltramiprosate) at Upcoming AD\/PD 2023 Conference in Gothenburg, Sweden - Pharma Trend<\/title>\n<meta name=\"robots\" content=\"index, follow, max-snippet:-1, max-image-preview:large, max-video-preview:-1\" \/>\n<link rel=\"canonical\" href=\"https:\/\/pharma-trend.com\/en\/alzheon-to-present-biomarker-brain-preservation-and-clinical-effects-of-oral-tablet-alz-801-valiltramiprosate-at-upcoming-ad-pd-2023-conference-in-gothenburg-sweden\/\" \/>\n<meta property=\"og:locale\" content=\"en_US\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"Alzheon to Present Biomarker, Brain Preservation and Clinical Effects of Oral Tablet ALZ-801 (Valiltramiprosate) at Upcoming AD\/PD 2023 Conference in Gothenburg, Sweden - Pharma Trend\" \/>\n<meta property=\"og:description\" content=\"Industry-Leading Results Position ALZ-801 to Potentially Become the First Oral Agent that Can Slow or Even Stop and Prevent Alzheimer\u2019s Pathology in Patients and Healthy Individuals at Risk for the Disease Robust Disease-Modifying Effects Observed Through 52 Weeks of Treatment with ALZ-801 Tablet in APOE4 Carriers with Early Alzheimer\u2019s Disease New Data Further Validate Alzheon ... 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