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Wikipedia

Lixisenatide

January 01, 1970

Lixisenatide (trade name Lyxumia in the European Union and Adlyxin in the U.S. and manufactured by Sanofi) is a once-daily injectable GLP-1 receptor agonist for the treatment of type 2 diabetes.

Lixisenatide
Clinical data
Trade namesLyxumia (EU), Adlyxin (US)
AHFS/Drugs.comMonograph
MedlinePlusa617005
License data
Pregnancy
category
  • AU: B3
Routes of
administration		Subcutaneous
ATC code
Legal status
Legal status
Identifiers
CAS Number
  • 320367-13-3
PubChem CID
  • 90472060
IUPHAR/BPS
  • 7387
DrugBank
  • DB09265
ChemSpider
  • 17295846
UNII
  • 74O62BB01U
KEGG
  • D09729
ChEBI
  • CHEBI:85662
ChEMBL
  • ChEMBL2108336
ECHA InfoCard100.210.612
Chemical and physical data
FormulaC215H347N61O65S
Molar mass4858.56 g·mol−1
3D model (JSmol)
  • Interactive image
  • CCC(C)C(C(=O)NC(CCC(=O)O)C(=O)NC(Cc1c[nH]c2c1cccc2)C(=O)NC(CC(C)C)C(=O)NC(CCCCN)C(=O)NC(CC(=O)N)C(=O)NCC(=O)NCC(=O)N3CCCC3C(=O)NC(CO)C(=O)NC(CO)C(=O)NCC(=O)NC(C)C(=O)N4CCCC4C(=O)N5CCCC5C(=O)NC(CO)C(=O)NC(CCCCN)C(=O)NC(CCCCN)C(=O)NC(CCCCN)C(=O)NC(CCCCN)C(=O)NC(CCCCN)C(=O)NC(CCCCN)C(=O)N)NC(=O)C(Cc6ccccc6)NC(=O)C(CC(C)C)NC(=O)C(CCCNC(=N)N)NC(=O)C(C(C)C)NC(=O)C(C)NC(=O)C(CCC(=O)O)NC(=O)C(CCC(=O)O)NC(=O)C(CCC(=O)O)NC(=O)C(CCSC)NC(=O)C(CCC(=O)N)NC(=O)C(CCCCN)NC(=O)C(CO)NC(=O)C(CC(C)C)NC(=O)C(CC(=O)O)NC(=O)C(CO)NC(=O)C(C(C)O)NC(=O)C(Cc7ccccc7)NC(=O)C(C(C)O)NC(=O)CNC(=O)C(CCC(=O)O)NC(=O)CNC(=O)C(Cc8cnc[nH]8)N
  • InChI=1S/C215H347N61O65S/c1-16-115(10)173(210(337)256-141(68-74-170(299)300)194(321)261-148(94-122-98-232-126-50-24-23-49-124(122)126)199(326)258-143(89-111(2)3)196(323)247-134(58-32-40-83-223)189(316)262-149(96-160(226)285)180(307)235-100-161(286)233-104-165(290)274-85-42-60-156(274)207(334)267-154(108-280)206(333)265-151(105-277)181(308)237-101-162(287)239-117(12)213(340)276-87-44-62-158(276)214(341)275-86-43-61-157(275)208(335)268-153(107-279)204(331)249-132(56-30-38-81-221)187(314)246-131(55-29-37-80-220)186(313)245-130(54-28-36-79-219)185(312)244-129(53-27-35-78-218)184(311)243-128(52-26-34-77-217)183(310)242-127(176(227)303)51-25-33-76-216)272-201(328)146(92-120-45-19-17-20-46-120)260-197(324)144(90-112(4)5)257-190(317)135(59-41-84-231-215(228)229)255-209(336)172(114(8)9)271-177(304)116(11)240-182(309)138(65-71-167(293)294)251-192(319)139(66-72-168(295)296)252-193(320)140(67-73-169(297)298)253-195(322)142(75-88-342-15)254-191(318)137(63-69-159(225)284)250-188(315)133(57-31-39-82-222)248-203(330)152(106-278)266-198(325)145(91-113(6)7)259-200(327)150(97-171(301)302)263-205(332)155(109-281)269-212(339)175(119(14)283)273-202(329)147(93-121-47-21-18-22-48-121)264-211(338)174(118(13)282)270-164(289)103-236-179(306)136(64-70-166(291)292)241-163(288)102-234-178(305)125(224)95-123-99-230-110-238-123/h17-24,45-50,98-99,110-119,125,127-158,172-175,232,277-283H,16,25-44,51-97,100-109,216-224H2,1-15H3,(H2,225,284)(H2,226,285)(H2,227,303)(H,230,238)(H,233,286)(H,234,305)(H,235,307)(H,236,306)(H,237,308)(H,239,287)(H,240,309)(H,241,288)(H,242,310)(H,243,311)(H,244,312)(H,245,313)(H,246,314)(H,247,323)(H,248,330)(H,249,331)(H,250,315)(H,251,319)(H,252,320)(H,253,322)(H,254,318)(H,255,336)(H,256,337)(H,257,317)(H,258,326)(H,259,327)(H,260,324)(H,261,321)(H,262,316)(H,263,332)(H,264,338)(H,265,333)(H,266,325)(H,267,334)(H,268,335)(H,269,339)(H,270,289)(H,271,304)(H,272,328)(H,273,329)(H,291,292)(H,293,294)(H,295,296)(H,297,298)(H,299,300)(H,301,302)(H4,228,229,231)/t115-,116-,117-,118+,119+,125-,127-,128-,129-,130-,131-,132-,133-,134-,135-,136-,137-,138-,139-,140-,141-,142-,143-,144-,145-,146-,147-,148-,149-,150-,151-,152-,153-,154-,155-,156-,157-,158-,172-,173-,174-,175-/m0/s1
  • Key:XVVOERDUTLJJHN-IAEQDCLQSA-N

Medical use edit

Lixisenatide is used as adjunct to diet and exercise to treat type 2 diabetes.[3] In the European Union, its use is limited to complementing insulin therapy.[2][4] As of 2017 it is unclear if they affect a person's risk of death.[5]

It is provided in an autoinjector containing fourteen doses and is injected subcutaneously.[3]

Lixisenatide should not be used for people who have problems with stomach emptying.[3] Lixisenatide delays emptying of the stomach, which may change how quickly other drugs that are taken by mouth take effect.[3]

Lixisenatide in neurodegenerative diseases edit

Results from a research work which was done by McClean PL et al. demonstrated that the GLP-1 receptor agonists liraglutide and lixisenatide which are on the market as treatments for type 2 diabetes show promise as potential drug treatments of Alzheimer disease AD. Lixisenatide was equally effective at a lower dose compared to liraglutide in some of the measured parameters after ten weeks of daily intraperitoneal injections with liraglutide (2.5 or 25 nmol/kg) or lixisenatide (1 or 10 nmol/kg) or saline of APP/PS1 mice at an age when amyloid plaques had already formed. When analyzing synaptic plasticity in the hippocampus, LTP was strongly increased in APP/PS1 mice by either drug, with more effectiveness accomplished with lixisenatide. The reduction of synapse numbers seen in APP/PS1 mice was prevented by the two drugs. The amyloid plaque load and dense-core Congo red positive plaque load in the cortex were reduced by both drugs at all doses. The chronic inflammation response (microglial activation) was also reduced by all treatments.[6]

Cai HY et al. demonstrated in a study that lixisenatide could reduce amyloid plaques, neurofibrillary tangles and neuroinflammation in the hippocampi of 12-month-old APP/PS1/tau female mice; activation of PKA-CREB signaling pathway and inhibition of p38-MAPK might be the important mechanisms in the neuroprotective function of lixisenatide. So, lixisenatide might have the potential to be developed as a novel therapy for AD.[7] Liu Wet al found an interesting results when comparing exendin-4 (10 nmol/kg), liraglutide (25 nmol/kg) and lixisenatide (10 nmol/kg), it was found that exendin-4 showed no protective effects at the dose chosen, while both liraglutide and lixisenatide showed effects in preventing the MPTP-induced motor impairment (Rotarod, open-field locomotion, catalepsy test), reduction in tyrosine hydroxylase (TH) levels (dopamine synthesis) in the substantia nigra and basal ganglia, a reduction of the pro-apoptotic signaling molecule BAX and an increase in the anti-apoptotic signaling molecule B-cell lymphoma-2. The previous results demonstrate that both liraglutide and lixisenatide are superior to exendin-4, and both drugs show promise as a novel treatment of Parkinson disease.[8]

Another study done by Kerry Hunter et al. profiled the GLP-1 receptor agonists liraglutide and lixisenatide. The kinetics of crossing the blood brain barrier (BBB), activation of the GLP-1R by measuring cAMP levels, and physiological effects in the brain on neuronal stem cell proliferation and neurogenesis were evaluated. Both drugs were able to cross the BBB. Lixisenatide crossed the BBB at all doses tested (2.5, 25, or 250 nmol/kg ip.) when measured 30 min post-injection and at 2.5-25 nmol/kg ip. 3 h post-injection. Lixisenatide also enhanced neurogenesis in the brain. Liraglutide crossed the BBB at 25 and 250 nmol/kg ip. but no increase was detectable at 2.5 nmol/kg ip. 30 min post-injection, and at 250 nmol/kg ip. at 3 h post-injection. Liraglutide and lixisenatide enhanced cAMP levels in the brain, with lixisenatide being more effective. The previous results suggest that these novel incretin analogues cross the BBB showing physiological activity and neurogenesis in the brain, which makes them good candidates to be used as a treatment of neurodegenerative diseases.[9]

Adverse effects edit

In about 0.1% of cases people have had anaphylactic reactions to lixisenatide and in about 0.2% of cases the drug has caused pancreatitis.[3] Use with insulin or sulfonylurea may cause hypoglycemia.[3] In some cases, people with no kidney disease have had acute kidney injury and in some people with existing kidney disease the condition has gotten worse.[3] Because lixisenatide is a peptide people can and do develop an immune response to it that will eventually make the drug ineffective; people who have developed antibodies to lixisenatide tend to have more inflammation at the injection site.[3]

At least 5% of people had nausea, vomiting, diarrhea, headache, or dizziness after taking lixisenatide.[3]

Mechanism of action edit

Lixisenatide is a member of the class of glucagon-like peptide-1 receptor agonist drugs, each of which activates the GLP-1 receptor. GLP-1 is a hormone that helps pancreatic beta cells to secrete insulin in response to high blood sugar. Because it works like the normal hormone, insulin is only secreted when blood sugar is high. Like GLP-1, it also slows gastric emptying.[2]

Chemistry edit

Lixisenatide is a peptide made of 44 amino acids, with an amide group on its C terminus.[3]

has been described as "des-38-proline-exendin-4 (Heloderma suspectum)-(1–39)-peptidylpenta-L-lysyl-L-lysinamide", meaning it is derived from the first 39 amino acids in the sequence of the peptide exendin-4, that was isolated from the Gila monster venom, omitting proline at position 38 and adding six lysine residues. Its complete sequence is:[10]

H–HisGlyGlu–Gly–ThrPhe–Thr–SerAspLeu–Ser–LysGlnMet–Glu–Glu–Glu–AlaValArg–Leu–Phe–Ile–Glu–Trp–Leu–Lys–Asn–Gly–Gly–Pro–Ser–Ser–Gly–Ala–Pro–Pro–Ser–Lys–Lys–Lys–Lys–Lys–Lys–NH2

History edit

It was created by Zealand Pharma A/S of Denmark;[11] in 2003 Zealand licensed it to Sanofi which developed the drug.[12] Lixisenatide was approved by the European Commission in February 2013.[2] Sanofi submitted an NDA in the US, which was accepted for review by the US FDA in February 2013,[13] but after discussions with the FDA about the cardiovascular safety data included in the package (starting in 2008, the FDA had required stronger CV safety data for new anti-diabetes drugs, following the controversy around the risks of Avandia)[14] Sanofi decided to withdraw the NDA and wait for the results of a Phase III study that was scheduled to be completed in 2015.[15][16] Because the drug was the first GLP-1 agonist that could be taken once a day, sales projections in 2013 were €500M per year by 2018.[16] Sanofi resubmitted the application which the FDA accepted in September 2015, by which time Sanofi had lost the lead in the field of anti-diabetic drugs to Novo Nordisk.[17] Lixisenatide received FDA approval in July 2016.[18]

In 2010, Zealand and Sanofi extended their license agreement to allow Sanofi to develop a combination therapy of lixisenatide with insulin glargine, which was Sanofi's best selling drug at the time, with sales of around €3 billion in 2009.[19] Sanofi planned to start the Phase III trial that year.[19] Sanofi submitted the NDA in December 2015, for the combination, called LixiLan and it was considered by the same Endocrinologic and Metabolic Drugs Advisory FDA Committee that was considering lixisenatide as a single agent.[20][21] In May 2016 by a vote of 12–2, with several members of the committee expressing reservations about Sanofi's plans to offer two pens with different ratios of insulin glargine and lixisenatide - one for people who had never taken insulin before and one for people who had; there was also concern about how to handle dosing when switching people from a single drug regimen to the combination drug.[20][22][23] In August 2016 the FDA told Sanofi that it was delaying a final decision for three months, and asked Sanofi for more data on how people used the delivery devices.[24]

Patent protection for lixisenatide expired in 2020.[25]

References edit

  1. ^ "Diabetic health". Health Canada. May 8, 2018. Retrieved April 13, 2024.
  2. ^ a b c d . UK Electronic Medicines Compendium. May 2, 2016. Archived from the original on September 23, 2016. Retrieved September 21, 2016.
  3. ^ a b c d e f g h i j k "Adlyxin- lixisenatide kit Adlyxin- lixisenatide injection, solution". DailyMed. January 11, 2019. Retrieved September 7, 2020.
  4. ^ a b "Lyxumia EPAR". European Medicines Agency (EMA). September 17, 2018. Retrieved September 7, 2020.
  5. ^ Liu J, Li L, Deng K, Xu C, Busse JW, Vandvik PO, et al. (June 2017). "Incretin based treatments and mortality in patients with type 2 diabetes: systematic review and meta-analysis". BMJ. 357: j2499. doi:10.1136/bmj.j2499. PMC 5463186. PMID 28596247.
  6. ^ McClean PL, Hölscher C (November 2014). "Lixisenatide, a drug developed to treat type 2 diabetes, shows neuroprotective effects in a mouse model of Alzheimer's disease". Neuropharmacology. 86: 241–58. doi:10.1016/j.neuropharm.2014.07.015. PMID 25107586. S2CID 24550291.
  7. ^ Cai HY, Yang JT, Wang ZJ, Zhang J, Yang W, Wu MN, Qi JS (January 2018). "Lixisenatide reduces amyloid plaques, neurofibrillary tangles and neuroinflammation in an APP/PS1/tau mouse model of Alzheimer's disease". Biochemical and Biophysical Research Communications. 495 (1): 1034–1040. doi:10.1016/j.bbrc.2017.11.114. PMID 29175324.
  8. ^ Liu W, Jalewa J, Sharma M, Li G, Li L, Hölscher C (September 2015). "Neuroprotective effects of lixisenatide and liraglutide in the 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine mouse model of Parkinson's disease" (PDF). Neuroscience. 303: 42–50. doi:10.1016/j.neuroscience.2015.06.054. PMID 26141845. S2CID 35297066.
  9. ^ Hunter K, Hölscher C (March 2012). "Drugs developed to treat diabetes, liraglutide and lixisenatide, cross the blood brain barrier and enhance neurogenesis". BMC Neuroscience. 13 (1): 33. doi:10.1186/1471-2202-13-33. PMC 3352246. PMID 22443187.
  10. ^ "International Nonproprietary Names for Pharmaceutical Substances (INN). Recommended INN: List 61" (PDF). WHO Drug Information. 23 (1): 66f. 2009.
  11. ^ Christensen M, Knop FK, Holst JJ, Vilsboll T (August 2009). "Lixisenatide, a novel GLP-1 receptor agonist for the treatment of type 2 diabetes mellitus". IDrugs. 12 (8): 503–13. PMID 19629885.
  12. ^ Terry M (November 5, 2015). "In Attempt to Bolster Sagging Diabetes Revenue Sanofi Inks Deal with Hanmi Pharma Worth 4 2 Billion". Biospace.
  13. ^ "Sanofi New Drug Application for Lixisenatide Accepted for Review by FDA". Drugs.com/PR Newsire. February 19, 2013.
  14. ^ Hughes S (July 3, 2008). "FDA Advisory Committee Recommends Cardiovascular Safety Studies for Diabetes Drugs". Medscape.
  15. ^ Nainggolan L (September 12, 2013). "Sanofi Withdraws US NDA for GLP-1 Agonist Lixisenatide". Medscape.
  16. ^ a b Humphreys A (December 1, 2013). "Reaching Epic Proportions 2013". PharmaLive.
  17. ^ Taylor P (September 30, 2015). "Sanofi's lixisenatide is back under FDA review". PM Live.
  18. ^ "FDA approves Adlyxin to treat type 2 diabetes". FDA. July 28, 2016. Retrieved July 28, 2016.
  19. ^ a b "Zealand extends Lixisenatide licence with S-A". PMLive. June 8, 2010.
  20. ^ a b Farooq R (May 24, 2016). . Business Finance News. Archived from the original on September 23, 2016.
  21. ^ "FDA Briefing Document Endocrinologic and Metabolic Drugs Advisory Committee Meeting" (PDF). FDA. May 25, 2016.
  22. ^ Nainggolan L (August 25, 2016). "Sanofi's GLP-1/Insulin Combo LixiLan Faces 3-Month Delay in US". Medscape.
  23. ^ "Summary Minutes of the Endocrinologic and Metabolic Drugs Advisory Committee Meeting" (PDF). FDA. May 25, 2016.
  24. ^ Staton T (August 21, 2016). "With FDA delay, Sanofi loses head start in diabetes combo-med rivalry with Novo". FiercePharma.
  25. ^ Elkinson S, Keating GM (March 2013). "Lixisenatide: first global approval". Drugs. 73 (4): 383–91. doi:10.1007/s40265-013-0033-3. PMID 23558600. S2CID 23612106.

January 01, 1970
lixisenatide, trade, name, lyxumia, european, union, adlyxin, manufactured, sanofi, once, daily, injectable, receptor, agonist, treatment, type, diabetes, clinical, datatrade, nameslyxumia, adlyxin, ahfs, drugs, commonographmedlineplusa617005license, dataus, d. Lixisenatide trade name Lyxumia in the European Union and Adlyxin in the U S and manufactured by Sanofi is a once daily injectable GLP 1 receptor agonist for the treatment of type 2 diabetes LixisenatideClinical dataTrade namesLyxumia EU Adlyxin US AHFS Drugs comMonographMedlinePlusa617005License dataUS DailyMed LixisenatidePregnancycategoryAU B3Routes ofadministrationSubcutaneousATC codeA10BJ03 WHO A10AE54 WHO Legal statusLegal statusCA only 1 UK POM Prescription only 2 US only 3 EU Rx only 4 IdentifiersCAS Number320367 13 3PubChem CID90472060IUPHAR BPS7387DrugBankDB09265ChemSpider17295846UNII74O62BB01UKEGGD09729ChEBICHEBI 85662ChEMBLChEMBL2108336ECHA InfoCard100 210 612Chemical and physical dataFormulaC 215H 347N 61O 65SMolar mass4858 56 g mol 13D model JSmol Interactive imageSMILES CCC C C C O NC CCC O O C O NC Cc1c nH c2c1cccc2 C O NC CC C C C O NC CCCCN C O NC CC O N C O NCC O NCC O N3CCCC3C O NC CO C O NC CO C O NCC O NC C C O N4CCCC4C O N5CCCC5C O NC CO C O NC CCCCN C O NC CCCCN C O NC CCCCN C O NC CCCCN C O NC CCCCN C O NC CCCCN C O N NC O C Cc6ccccc6 NC O C CC C C NC O C CCCNC N N NC O C C C C NC O C C NC O C CCC O O NC O C CCC O O NC O C CCC O O NC O C CCSC NC O C CCC O N NC O C CCCCN NC O C CO NC O C CC C C NC O C CC O O NC O C CO NC O C C C O NC O C Cc7ccccc7 NC O C C C O NC O CNC O C CCC O O NC O CNC O C Cc8cnc nH 8 NInChI InChI 1S C215H347N61O65S c1 16 115 10 173 210 337 256 141 68 74 170 299 300 194 321 261 148 94 122 98 232 126 50 24 23 49 124 122 126 199 326 258 143 89 111 2 3 196 323 247 134 58 32 40 83 223 189 316 262 149 96 160 226 285 180 307 235 100 161 286 233 104 165 290 274 85 42 60 156 274 207 334 267 154 108 280 206 333 265 151 105 277 181 308 237 101 162 287 239 117 12 213 340 276 87 44 62 158 276 214 341 275 86 43 61 157 275 208 335 268 153 107 279 204 331 249 132 56 30 38 81 221 187 314 246 131 55 29 37 80 220 186 313 245 130 54 28 36 79 219 185 312 244 129 53 27 35 78 218 184 311 243 128 52 26 34 77 217 183 310 242 127 176 227 303 51 25 33 76 216 272 201 328 146 92 120 45 19 17 20 46 120 260 197 324 144 90 112 4 5 257 190 317 135 59 41 84 231 215 228 229 255 209 336 172 114 8 9 271 177 304 116 11 240 182 309 138 65 71 167 293 294 251 192 319 139 66 72 168 295 296 252 193 320 140 67 73 169 297 298 253 195 322 142 75 88 342 15 254 191 318 137 63 69 159 225 284 250 188 315 133 57 31 39 82 222 248 203 330 152 106 278 266 198 325 145 91 113 6 7 259 200 327 150 97 171 301 302 263 205 332 155 109 281 269 212 339 175 119 14 283 273 202 329 147 93 121 47 21 18 22 48 121 264 211 338 174 118 13 282 270 164 289 103 236 179 306 136 64 70 166 291 292 241 163 288 102 234 178 305 125 224 95 123 99 230 110 238 123 h17 24 45 50 98 99 110 119 125 127 158 172 175 232 277 283H 16 25 44 51 97 100 109 216 224H2 1 15H3 H2 225 284 H2 226 285 H2 227 303 H 230 238 H 233 286 H 234 305 H 235 307 H 236 306 H 237 308 H 239 287 H 240 309 H 241 288 H 242 310 H 243 311 H 244 312 H 245 313 H 246 314 H 247 323 H 248 330 H 249 331 H 250 315 H 251 319 H 252 320 H 253 322 H 254 318 H 255 336 H 256 337 H 257 317 H 258 326 H 259 327 H 260 324 H 261 321 H 262 316 H 263 332 H 264 338 H 265 333 H 266 325 H 267 334 H 268 335 H 269 339 H 270 289 H 271 304 H 272 328 H 273 329 H 291 292 H 293 294 H 295 296 H 297 298 H 299 300 H 301 302 H4 228 229 231 t115 116 117 118 119 125 127 128 129 130 131 132 133 134 135 136 137 138 139 140 141 142 143 144 145 146 147 148 149 150 151 152 153 154 155 156 157 158 172 173 174 175 m0 s1Key XVVOERDUTLJJHN IAEQDCLQSA N Contents 1 Medical use 1 1 Lixisenatide in neurodegenerative diseases 2 Adverse effects 3 Mechanism of action 4 Chemistry 5 History 6 ReferencesMedical use editLixisenatide is used as adjunct to diet and exercise to treat type 2 diabetes 3 In the European Union its use is limited to complementing insulin therapy 2 4 As of 2017 it is unclear if they affect a person s risk of death 5 It is provided in an autoinjector containing fourteen doses and is injected subcutaneously 3 Lixisenatide should not be used for people who have problems with stomach emptying 3 Lixisenatide delays emptying of the stomach which may change how quickly other drugs that are taken by mouth take effect 3 Lixisenatide in neurodegenerative diseases edit Results from a research work which was done by McClean PL et al demonstrated that the GLP 1 receptor agonists liraglutide and lixisenatide which are on the market as treatments for type 2 diabetes show promise as potential drug treatments of Alzheimer disease AD Lixisenatide was equally effective at a lower dose compared to liraglutide in some of the measured parameters after ten weeks of daily intraperitoneal injections with liraglutide 2 5 or 25 nmol kg or lixisenatide 1 or 10 nmol kg or saline of APP PS1 mice at an age when amyloid plaques had already formed When analyzing synaptic plasticity in the hippocampus LTP was strongly increased in APP PS1 mice by either drug with more effectiveness accomplished with lixisenatide The reduction of synapse numbers seen in APP PS1 mice was prevented by the two drugs The amyloid plaque load and dense core Congo red positive plaque load in the cortex were reduced by both drugs at all doses The chronic inflammation response microglial activation was also reduced by all treatments 6 Cai HY et al demonstrated in a study that lixisenatide could reduce amyloid plaques neurofibrillary tangles and neuroinflammation in the hippocampi of 12 month old APP PS1 tau female mice activation of PKA CREB signaling pathway and inhibition of p38 MAPK might be the important mechanisms in the neuroprotective function of lixisenatide So lixisenatide might have the potential to be developed as a novel therapy for AD 7 Liu Wet al found an interesting results when comparing exendin 4 10 nmol kg liraglutide 25 nmol kg and lixisenatide 10 nmol kg it was found that exendin 4 showed no protective effects at the dose chosen while both liraglutide and lixisenatide showed effects in preventing the MPTP induced motor impairment Rotarod open field locomotion catalepsy test reduction in tyrosine hydroxylase TH levels dopamine synthesis in the substantia nigra and basal ganglia a reduction of the pro apoptotic signaling molecule BAX and an increase in the anti apoptotic signaling molecule B cell lymphoma 2 The previous results demonstrate that both liraglutide and lixisenatide are superior to exendin 4 and both drugs show promise as a novel treatment of Parkinson disease 8 Another study done by Kerry Hunter et al profiled the GLP 1 receptor agonists liraglutide and lixisenatide The kinetics of crossing the blood brain barrier BBB activation of the GLP 1R by measuring cAMP levels and physiological effects in the brain on neuronal stem cell proliferation and neurogenesis were evaluated Both drugs were able to cross the BBB Lixisenatide crossed the BBB at all doses tested 2 5 25 or 250 nmol kg ip when measured 30 min post injection and at 2 5 25 nmol kg ip 3 h post injection Lixisenatide also enhanced neurogenesis in the brain Liraglutide crossed the BBB at 25 and 250 nmol kg ip but no increase was detectable at 2 5 nmol kg ip 30 min post injection and at 250 nmol kg ip at 3 h post injection Liraglutide and lixisenatide enhanced cAMP levels in the brain with lixisenatide being more effective The previous results suggest that these novel incretin analogues cross the BBB showing physiological activity and neurogenesis in the brain which makes them good candidates to be used as a treatment of neurodegenerative diseases 9 Adverse effects editIn about 0 1 of cases people have had anaphylactic reactions to lixisenatide and in about 0 2 of cases the drug has caused pancreatitis 3 Use with insulin or sulfonylurea may cause hypoglycemia 3 In some cases people with no kidney disease have had acute kidney injury and in some people with existing kidney disease the condition has gotten worse 3 Because lixisenatide is a peptide people can and do develop an immune response to it that will eventually make the drug ineffective people who have developed antibodies to lixisenatide tend to have more inflammation at the injection site 3 At least 5 of people had nausea vomiting diarrhea headache or dizziness after taking lixisenatide 3 Mechanism of action editLixisenatide is a member of the class of glucagon like peptide 1 receptor agonist drugs each of which activates the GLP 1 receptor GLP 1 is a hormone that helps pancreatic beta cells to secrete insulin in response to high blood sugar Because it works like the normal hormone insulin is only secreted when blood sugar is high Like GLP 1 it also slows gastric emptying 2 Chemistry editLixisenatide is a peptide made of 44 amino acids with an amide group on its C terminus 3 has been described as des 38 proline exendin 4 Heloderma suspectum 1 39 peptidylpenta L lysyl L lysinamide meaning it is derived from the first 39 amino acids in the sequence of the peptide exendin 4 that was isolated from the Gila monster venom omitting proline at position 38 and adding six lysine residues Its complete sequence is 10 H His Gly Glu Gly Thr Phe Thr Ser Asp Leu Ser Lys Gln Met Glu Glu Glu Ala Val Arg Leu Phe Ile Glu Trp Leu Lys Asn Gly Gly Pro Ser Ser Gly Ala Pro Pro Ser Lys Lys Lys Lys Lys Lys NH2History editIt was created by Zealand Pharma A S of Denmark 11 in 2003 Zealand licensed it to Sanofi which developed the drug 12 Lixisenatide was approved by the European Commission in February 2013 2 Sanofi submitted an NDA in the US which was accepted for review by the US FDA in February 2013 13 but after discussions with the FDA about the cardiovascular safety data included in the package starting in 2008 the FDA had required stronger CV safety data for new anti diabetes drugs following the controversy around the risks of Avandia 14 Sanofi decided to withdraw the NDA and wait for the results of a Phase III study that was scheduled to be completed in 2015 15 16 Because the drug was the first GLP 1 agonist that could be taken once a day sales projections in 2013 were 500M per year by 2018 16 Sanofi resubmitted the application which the FDA accepted in September 2015 by which time Sanofi had lost the lead in the field of anti diabetic drugs to Novo Nordisk 17 Lixisenatide received FDA approval in July 2016 18 In 2010 Zealand and Sanofi extended their license agreement to allow Sanofi to develop a combination therapy of lixisenatide with insulin glargine which was Sanofi s best selling drug at the time with sales of around 3 billion in 2009 19 Sanofi planned to start the Phase III trial that year 19 Sanofi submitted the NDA in December 2015 for the combination called LixiLan and it was considered by the same Endocrinologic and Metabolic Drugs Advisory FDA Committee that was considering lixisenatide as a single agent 20 21 In May 2016 by a vote of 12 2 with several members of the committee expressing reservations about Sanofi s plans to offer two pens with different ratios of insulin glargine and lixisenatide one for people who had never taken insulin before and one for people who had there was also concern about how to handle dosing when switching people from a single drug regimen to the combination drug 20 22 23 In August 2016 the FDA told Sanofi that it was delaying a final decision for three months and asked Sanofi for more data on how people used the delivery devices 24 Patent protection for lixisenatide expired in 2020 25 References edit Diabetic health Health Canada May 8 2018 Retrieved April 13 2024 a b c d Lyxumia 10 micrograms solution for injection Summary of Product Characteristics SPC UK Electronic Medicines Compendium May 2 2016 Archived from the original on September 23 2016 Retrieved September 21 2016 a b c d e f g h i j k Adlyxin lixisenatide kit Adlyxin lixisenatide injection solution DailyMed January 11 2019 Retrieved September 7 2020 a b Lyxumia EPAR European Medicines Agency EMA September 17 2018 Retrieved September 7 2020 Liu J Li L Deng K Xu C Busse JW Vandvik PO et al June 2017 Incretin based treatments and mortality in patients with type 2 diabetes systematic review and meta analysis BMJ 357 j2499 doi 10 1136 bmj j2499 PMC 5463186 PMID 28596247 McClean PL Holscher C November 2014 Lixisenatide a drug developed to treat type 2 diabetes shows neuroprotective effects in a mouse model of Alzheimer s disease Neuropharmacology 86 241 58 doi 10 1016 j neuropharm 2014 07 015 PMID 25107586 S2CID 24550291 Cai HY Yang JT Wang ZJ Zhang J Yang W Wu MN Qi JS January 2018 Lixisenatide reduces amyloid plaques neurofibrillary tangles and neuroinflammation in an APP PS1 tau mouse model of Alzheimer s disease Biochemical and Biophysical Research Communications 495 1 1034 1040 doi 10 1016 j bbrc 2017 11 114 PMID 29175324 Liu W Jalewa J Sharma M Li G Li L Holscher C September 2015 Neuroprotective effects of lixisenatide and liraglutide in the 1 methyl 4 phenyl 1 2 3 6 tetrahydropyridine mouse model of Parkinson s disease PDF Neuroscience 303 42 50 doi 10 1016 j neuroscience 2015 06 054 PMID 26141845 S2CID 35297066 Hunter K Holscher C March 2012 Drugs developed to treat diabetes liraglutide and lixisenatide cross the blood brain barrier and enhance neurogenesis BMC Neuroscience 13 1 33 doi 10 1186 1471 2202 13 33 PMC 3352246 PMID 22443187 International Nonproprietary Names for Pharmaceutical Substances INN Recommended INN List 61 PDF WHO Drug Information 23 1 66f 2009 Christensen M Knop FK Holst JJ Vilsboll T August 2009 Lixisenatide a novel GLP 1 receptor agonist for the treatment of type 2 diabetes mellitus IDrugs 12 8 503 13 PMID 19629885 Terry M November 5 2015 In Attempt to Bolster Sagging Diabetes Revenue Sanofi Inks Deal with Hanmi Pharma Worth 4 2 Billion Biospace Sanofi New Drug Application for Lixisenatide Accepted for Review by FDA Drugs com PR Newsire February 19 2013 Hughes S July 3 2008 FDA Advisory Committee Recommends Cardiovascular Safety Studies for Diabetes Drugs Medscape Nainggolan L September 12 2013 Sanofi Withdraws US NDA for GLP 1 Agonist Lixisenatide Medscape a b Humphreys A December 1 2013 Reaching Epic Proportions 2013 PharmaLive Taylor P September 30 2015 Sanofi s lixisenatide is back under FDA review PM Live FDA approves Adlyxin to treat type 2 diabetes FDA July 28 2016 Retrieved July 28 2016 a b Zealand extends Lixisenatide licence with S A PMLive June 8 2010 a b Farooq R May 24 2016 Sanofi SA ADR and Diabetes Things Are Not Working Out Business Finance News Archived from the original on September 23 2016 FDA Briefing Document Endocrinologic and Metabolic Drugs Advisory Committee Meeting PDF FDA May 25 2016 Nainggolan L August 25 2016 Sanofi s GLP 1 Insulin Combo LixiLan Faces 3 Month Delay in US Medscape Summary Minutes of the Endocrinologic and Metabolic Drugs Advisory Committee Meeting PDF FDA May 25 2016 Staton T August 21 2016 With FDA delay Sanofi loses head start in diabetes combo med rivalry with Novo FiercePharma Elkinson S Keating GM March 2013 Lixisenatide first global approval Drugs 73 4 383 91 doi 10 1007 s40265 013 0033 3 PMID 23558600 S2CID 23612106 Portal nbsp Medicine Retrieved from https en wikipedia org w index php title Lixisenatide amp oldid 1218743279, wikipedia, wiki, book, books, library,

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