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PMC:7696151 / 41351-66061 JSONTXT

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LitCovid-PubTator

Id Subject Object Predicate Lexical cue tao:has_database_id
1165 5-23 Chemical denotes Hydroxychloroquine MESH:D006886
1167 75-78 Chemical denotes HCQ MESH:D006886
1175 432-435 Chemical denotes HCQ MESH:D006886
1176 319-339 Disease denotes rheumatoid arthritis MESH:D001172
1177 341-360 Disease denotes lupus erythematosus MESH:D008180
1178 370-388 Disease denotes Sjögren’s syndrome MESH:D012859
1179 513-570 Disease denotes autoimmune disease-dependent cardiovascular complications MESH:D002318
1180 637-650 Disease denotes hyperglycemia MESH:D006943
1181 652-666 Disease denotes hyperlipidemia MESH:D006949
1191 701-704 Chemical denotes HCQ MESH:D006886
1192 1091-1094 Chemical denotes HCQ MESH:D006886
1193 1291-1294 Chemical denotes HCQ MESH:D006886
1194 1360-1363 Chemical denotes HCQ MESH:D006886
1195 1499-1502 Chemical denotes HCQ MESH:D006886
1196 835-843 Disease denotes toxicity MESH:D064420
1197 941-949 Disease denotes toxicity MESH:D064420
1198 1393-1405 Disease denotes inflammation MESH:D007249
1199 1415-1423 Disease denotes toxicity MESH:D064420
1201 1569-1589 Disease denotes Rheumatoid Arthritis MESH:D001172
1216 2024-2029 Species denotes women Tax:9606
1217 2420-2424 Species denotes rats Tax:10116
1218 2070-2073 Chemical denotes HCQ MESH:D006886
1219 2382-2385 Chemical denotes HCQ MESH:D006886
1220 1590-1610 Disease denotes Rheumatoid arthritis MESH:D001172
1221 1625-1643 Disease denotes autoimmune disease MESH:D001327
1222 1670-1682 Disease denotes inflammation MESH:D007249
1223 1760-1780 Disease denotes rheumatoid arthritis MESH:D001172
1224 1839-1849 Disease denotes rheumatoid MESH:D011695
1225 1979-1999 Disease denotes rheumatoid arthritis MESH:D001172
1226 2127-2140 Disease denotes hyperactivity MESH:D006948
1227 2264-2273 Disease denotes Jancinova
1228 2439-2448 Disease denotes arthritis MESH:D001168
1229 2643-2655 Disease denotes inflammation MESH:D007249
1246 2836-2844 Species denotes patients Tax:9606
1247 3286-3294 Species denotes patients Tax:9606
1248 3495-3503 Species denotes patients Tax:9606
1249 3891-3899 Species denotes patients Tax:9606
1250 2773-2776 Chemical denotes HCQ MESH:D006886
1251 2910-2913 Chemical denotes HCQ MESH:D006886
1252 3074-3077 Chemical denotes HCQ MESH:D006886
1253 3306-3319 Chemical denotes sulfasalazine MESH:D012460
1254 3324-3327 Chemical denotes HCQ MESH:D006886
1255 3351-3354 Chemical denotes HCQ MESH:D006886
1256 3431-3444 Chemical denotes sulfasalazine MESH:D012460
1257 3517-3520 Chemical denotes HCQ MESH:D006886
1258 2850-2870 Disease denotes rheumatoid arthritis MESH:D001172
1259 2988-2997 Disease denotes synovitis MESH:D013585
1260 3002-3012 Disease denotes joint pain MESH:D018771
1261 3672-3676 Disease denotes pain MESH:D010146
1303 4224-4228 Gene denotes IL-6 Gene:3569
1304 4382-4388 Gene denotes leptin Gene:3952
1305 4515-4519 Gene denotes IL-6 Gene:3569
1306 4524-4530 Gene denotes leptin Gene:3952
1307 5693-5700 Gene denotes insulin Gene:3630
1308 5760-5767 Gene denotes insulin Gene:3630
1309 3909-3917 Species denotes patients Tax:9606
1310 4732-4740 Species denotes patients Tax:9606
1311 5095-5103 Species denotes patients Tax:9606
1312 5261-5266 Species denotes women Tax:9606
1313 5363-5368 Species denotes women Tax:9606
1314 5657-5665 Species denotes patients Tax:9606
1315 6033-6041 Species denotes patients Tax:9606
1316 4252-4257 Chemical denotes lipid MESH:D008055
1317 4491-4494 Chemical denotes HCQ MESH:D006886
1318 4562-4565 Chemical denotes HCQ MESH:D006886
1319 4775-4786 Chemical denotes cholesterol MESH:D002784
1320 4839-4851 Chemical denotes triglyceride MESH:D014280
1321 4877-4880 Chemical denotes HCQ MESH:D006886
1322 4965-4976 Chemical denotes cholesterol MESH:D002784
1323 4991-4994 Chemical denotes HCQ MESH:D006886
1324 5160-5163 Chemical denotes HCQ MESH:D006886
1325 5321-5324 Chemical denotes HCQ MESH:D006886
1326 5352-5359 Chemical denotes glucose MESH:D005947
1327 5626-5629 Chemical denotes HCQ MESH:D006886
1328 6002-6005 Chemical denotes HCQ MESH:D006886
1329 3923-3943 Disease denotes rheumatoid arthritis MESH:D001172
1330 4090-4105 Disease denotes atherosclerotic MESH:D050197
1331 4155-4167 Disease denotes hypertension MESH:D006973
1332 4169-4176 Disease denotes obesity MESH:D009765
1333 4182-4200 Disease denotes metabolic syndrome MESH:D024821
1334 4327-4339 Disease denotes inflammation MESH:D007249
1335 4569-4581 Disease denotes dyslipidemia MESH:D050171
1336 4701-4721 Disease denotes rheumatoid arthritis MESH:D001172
1337 5109-5129 Disease denotes rheumatoid arthritis MESH:D001172
1338 5272-5292 Disease denotes rheumatoid arthritis MESH:D001172
1339 5547-5555 Disease denotes diabetic MESH:D003920
1340 5577-5597 Disease denotes rheumatoid arthritis MESH:D001172
1341 5847-5865 Disease denotes insulin metabolism MESH:D008659
1342 5979-5987 Disease denotes diabetic MESH:D003920
1343 6050-6059 Disease denotes arthritis MESH:D001168
1345 6105-6124 Disease denotes Lupus Erythematosus MESH:D008180
1393 9736-9740 Gene denotes IL-6 Gene:3569
1394 9745-9750 Gene denotes TNF-α Gene:7124
1395 9988-9993 Gene denotes IFN-α Gene:3439
1396 8597-8600 Gene denotes lpr Gene:14102
1397 7034-7042 Species denotes patients Tax:9606
1398 7065-7071 Species denotes People Tax:9606
1399 7304-7312 Species denotes patients Tax:9606
1400 8601-8605 Species denotes mice Tax:10090
1401 9339-9347 Species denotes patients Tax:9606
1402 9796-9804 Species denotes patients Tax:9606
1403 6305-6308 Chemical denotes HCQ MESH:D006886
1404 6415-6418 Chemical denotes HCQ MESH:D006886
1405 6620-6623 Chemical denotes HCQ MESH:D006886
1406 6924-6927 Chemical denotes HCQ MESH:D006886
1407 7267-7270 Chemical denotes HCQ MESH:D006886
1408 7373-7376 Chemical denotes HCQ MESH:D006886
1409 7486-7489 Chemical denotes HCQ MESH:D006886
1410 7573-7576 Chemical denotes HCQ MESH:D006886
1411 7802-7805 Chemical denotes HCQ MESH:D006886
1412 8088-8091 Chemical denotes HCQ MESH:D006886
1413 8476-8479 Chemical denotes HCQ MESH:D006886
1414 8563-8566 Chemical denotes HCQ MESH:D006886
1415 8666-8669 Chemical denotes HCQ MESH:D006886
1416 8754-8758 Chemical denotes Treg
1417 9114-9117 Chemical denotes HCQ MESH:D006886
1418 9401-9404 Chemical denotes HCQ MESH:D006886
1419 9560-9563 Chemical denotes HCQ MESH:D006886
1420 9806-9809 Chemical denotes HCQ MESH:D006886
1421 6134-6153 Disease denotes lupus erythematosus MESH:D008180
1422 6159-6213 Disease denotes multisystemic autoimmune chronic inflammatory disorder MESH:D019693
1423 6448-6467 Disease denotes lupus erythematosus MESH:D008180
1424 6793-6803 Disease denotes thrombotic MESH:D013927
1425 7058-7063 Disease denotes lupus MESH:D008180
1426 7161-7172 Disease denotes skin rashes MESH:D005076
1427 7174-7183 Disease denotes arthritis MESH:D001168
1428 7189-7195 Disease denotes ulcers MESH:D014456
1429 7284-7303 Disease denotes lupus erythematosus MESH:D008180
1430 7533-7538 Disease denotes lupus MESH:D008180
1431 7695-7700 Disease denotes lupus MESH:D008180
1432 8335-8354 Disease denotes autoimmune diseases MESH:D001327
1433 8373-8378 Disease denotes lupus MESH:D008180
1434 8615-8633 Disease denotes lupus-like disease MESH:D008180
1435 9144-9174 Disease denotes attenuated kidney inflammation MESH:C538265
1436 9368-9373 Disease denotes lupus MESH:D008180
1437 9510-9523 Disease denotes lupus disease MESH:D008180
1438 9790-9795 Disease denotes lupus MESH:D008180
1439 10025-10030 Disease denotes lupus MESH:D008180
1450 10261-10264 Gene denotes lpr Gene:14102
1451 10265-10271 Species denotes murine Tax:10090
1452 10202-10205 Chemical denotes HCQ MESH:D006886
1453 10408-10413 Chemical denotes water MESH:D014867
1454 10684-10687 Chemical denotes HCQ MESH:D006886
1455 10162-10167 Disease denotes lupus MESH:D008180
1456 10169-10180 Disease denotes skin rashes MESH:D005076
1457 10281-10286 Disease denotes lupus MESH:D008180
1458 10481-10490 Disease denotes mortality MESH:D003643
1459 10711-10745 Disease denotes skin injury in lupus erythematosus MESH:D008180
1504 12546-12553 Gene denotes insulin Gene:3630
1505 11053-11057 Species denotes mice Tax:10090
1506 11484-11490 Species denotes murine Tax:10090
1507 11750-11758 Species denotes patients Tax:9606
1508 11962-11970 Species denotes patients Tax:9606
1509 12086-12094 Species denotes patients Tax:9606
1510 12385-12393 Species denotes patients Tax:9606
1511 12470-12475 Species denotes women Tax:9606
1512 11079-11082 Chemical denotes HCQ MESH:D006886
1513 11324-11347 Chemical denotes Reactive Oxygen Species MESH:D017382
1514 11349-11352 Chemical denotes ROS MESH:D017382
1515 11370-11373 Chemical denotes HCQ MESH:D006886
1516 11418-11430 Chemical denotes nitric oxide MESH:D009569
1517 11435-11438 Chemical denotes ROS MESH:D017382
1518 11517-11520 Chemical denotes HCQ MESH:D006886
1519 11686-11691 Chemical denotes lipid MESH:D008055
1520 11710-11713 Chemical denotes HCQ MESH:D006886
1521 11816-11819 Chemical denotes HCQ MESH:D006886
1522 11852-11864 Chemical denotes triglyceride MESH:D014280
1523 11869-11880 Chemical denotes cholesterol MESH:D002784
1524 11955-11958 Chemical denotes HCQ MESH:D006886
1525 12035-12040 Chemical denotes lipid MESH:D008055
1526 12109-12112 Chemical denotes HCQ MESH:D006886
1527 12155-12168 Chemical denotes triglycerides MESH:D014280
1528 12252-12263 Chemical denotes cholesterol MESH:D002784
1529 12289-12292 Chemical denotes HCQ MESH:D006886
1530 12534-12537 Chemical denotes HCQ MESH:D006886
1531 12628-12635 Chemical denotes glucose MESH:D005947
1532 10798-10817 Disease denotes lupus erythematosus MESH:D008180
1533 10854-10882 Disease denotes cardiovascular complications MESH:D002318
1534 10925-10948 Disease denotes endothelial dysfunction MESH:C536439
1535 10973-10995 Disease denotes cardiovascular disease MESH:D002318
1536 11008-11020 Disease denotes hypertension MESH:D006973
1537 11025-11037 Disease denotes renal damage MESH:D007674
1538 11067-11072 Disease denotes lupus MESH:D008180
1539 11146-11160 Disease denotes thromboembolic MESH:D013923
1540 11195-11207 Disease denotes hypertension MESH:D006973
1541 11209-11221 Disease denotes renal damage MESH:D007674
1542 11227-11244 Disease denotes heart hypertrophy MESH:D006332
1543 11602-11625 Disease denotes endothelial dysfunction MESH:C536439
1544 11648-11663 Disease denotes atherosclerosis MESH:D050197
1545 12080-12085 Disease denotes lupus MESH:D008180
1546 12379-12384 Disease denotes lupus MESH:D008180
1547 12488-12493 Disease denotes lupus MESH:D008180
1563 12713-12721 Species denotes patients Tax:9606
1564 13067-13072 Species denotes women Tax:9606
1565 13102-13108 Species denotes people Tax:9606
1566 13421-13426 Species denotes women Tax:9606
1567 13566-13574 Species denotes patients Tax:9606
1568 12649-12652 Chemical denotes HCQ MESH:D006886
1569 12846-12849 Chemical denotes HCQ MESH:D006886
1570 12946-12956 Chemical denotes prednisone MESH:D011241
1571 13014-13017 Chemical denotes HCQ MESH:D006886
1572 13126-13129 Chemical denotes HCQ MESH:D006886
1573 13581-13584 Chemical denotes HCQ MESH:D006886
1574 12707-12712 Disease denotes lupus MESH:D008180
1575 13037-13042 Disease denotes lupus MESH:D008180
1576 13325-13333 Disease denotes toxicity MESH:D064420
1577 13432-13447 Disease denotes lupus nephritis MESH:D008181
1579 13657-13682 Disease denotes Antiphospholipid Syndrome MESH:D016736
1609 15600-15613 Gene denotes tissue factor Gene:2152
1610 13930-13935 Species denotes women Tax:9606
1611 14388-14393 Species denotes mouse Tax:10090
1612 14488-14493 Species denotes mouse Tax:10090
1613 14651-14656 Species denotes woman Tax:9606
1614 15277-15281 Species denotes mice Tax:10090
1615 15650-15658 Species denotes patients Tax:9606
1616 14342-14345 Chemical denotes HCQ MESH:D006886
1617 14440-14443 Chemical denotes HCQ MESH:D006886
1618 14633-14636 Chemical denotes HCQ MESH:D006886
1619 14721-14724 Chemical denotes HCQ MESH:D006886
1620 14784-14787 Chemical denotes HCQ MESH:D006886
1621 14823-14830 Chemical denotes aspirin MESH:D001241
1622 14835-14842 Chemical denotes heparin MESH:D006493
1623 15005-15008 Chemical denotes HCQ MESH:D006886
1624 15124-15127 Chemical denotes HCQ MESH:D006886
1625 15175-15178 Chemical denotes HCQ MESH:D006886
1626 15454-15457 Chemical denotes HCQ MESH:D006886
1627 15540-15543 Chemical denotes HCQ MESH:D006886
1628 15741-15744 Chemical denotes HCQ MESH:D006886
1629 13683-13708 Disease denotes Antiphospholipid syndrome MESH:D016736
1630 13715-13734 Disease denotes autoimmune disorder MESH:D001327
1631 13831-13850 Disease denotes autoimmune diseases MESH:D001327
1632 14403-14438 Disease denotes obstetric antiphospholipid syndrome MESH:D016736
1633 14672-14694 Disease denotes venous thromboembolism MESH:D054556
1634 14889-14899 Disease denotes thrombosis MESH:D013927
1635 15256-15273 Disease denotes thrombotic status MESH:D013927
1636 15292-15317 Disease denotes antiphospholipid syndrome MESH:D016736
1637 15664-15689 Disease denotes antiphospholipid syndrome MESH:D016736
1669 17205-17210 Gene denotes TGF-β Gene:7039
1670 17212-17240 Gene denotes transforming growth factor-β Gene:7124
1671 17276-17281 Gene denotes TGF-β Gene:21802
1672 15893-15899 Species denotes people Tax:9606
1673 16886-16891 Species denotes women Tax:9606
1674 17068-17076 Species denotes patients Tax:9606
1675 17318-17322 Species denotes mice Tax:10090
1676 17752-17756 Species denotes mice Tax:10090
1677 16065-16068 Chemical denotes HCQ MESH:D006886
1678 16527-16530 Chemical denotes HCQ MESH:D006886
1679 16635-16638 Chemical denotes HCQ MESH:D006886
1680 16931-16934 Chemical denotes HCQ MESH:D006886
1681 16991-16994 Chemical denotes HCQ MESH:D006886
1682 17258-17261 Chemical denotes HCQ MESH:D006886
1683 17476-17479 Chemical denotes HCQ MESH:D006886
1684 17687-17690 Chemical denotes HCQ MESH:D006886
1685 15769-15802 Disease denotes Sjögren Syndrome Sjögren syndrome MESH:D012859
1686 15809-15827 Disease denotes autoimmune disease MESH:D001327
1687 15938-15962 Disease denotes lymphocytic inflammation MESH:D007249
1688 16013-16023 Disease denotes xerostomia MESH:D014987
1689 16076-16092 Disease denotes Sjögren syndrome MESH:D012859
1690 16548-16564 Disease denotes Sjögren syndrome MESH:D012859
1691 16869-16885 Disease denotes Sjögren syndrome MESH:D012859
1692 16961-16972 Disease denotes eye dryness MESH:D014987
1693 17084-17099 Disease denotes Hypo-salivation MESH:D052456
1694 17114-17128 Disease denotes acinar atrophy MESH:D018267
1695 17133-17141 Disease denotes fibrosis MESH:D005355
1696 17561-17585 Disease denotes lymphocytic infiltration MESH:D017254
1697 17770-17794 Disease denotes lymphocytic infiltration MESH:D017254
1699 17894-17902 Disease denotes Diabetes MESH:D003920
1744 18280-18287 Gene denotes insulin Gene:3630
1745 18669-18676 Gene denotes insulin Gene:3630
1746 19414-19421 Gene denotes insulin Gene:3630
1747 19697-19704 Gene denotes insulin Gene:3630
1748 17951-17959 Species denotes patients Tax:9606
1749 18175-18179 Species denotes rats Tax:10116
1750 18466-18470 Species denotes rats Tax:10116
1751 18603-18607 Species denotes rats Tax:10116
1752 18700-18704 Species denotes rats Tax:10116
1753 19053-19061 Species denotes patients Tax:9606
1754 19867-19875 Species denotes patients Tax:9606
1755 17961-17964 Chemical denotes HCQ MESH:D006886
1756 18042-18045 Chemical denotes HCQ MESH:D006886
1757 18237-18240 Chemical denotes HCQ MESH:D006886
1758 18333-18340 Chemical denotes glucose MESH:D005947
1759 18372-18375 Chemical denotes HCQ MESH:D006886
1760 18483-18486 Chemical denotes HCQ MESH:D006886
1761 18662-18665 Chemical denotes HCQ MESH:D006886
1762 18888-18891 Chemical denotes HCQ MESH:D006886
1763 19013-19016 Chemical denotes HCQ MESH:D006886
1764 19063-19066 Chemical denotes HCQ MESH:D006886
1765 19354-19357 Chemical denotes HCQ MESH:D006886
1766 19596-19599 Chemical denotes HCQ MESH:D006886
1767 19748-19751 Chemical denotes HCQ MESH:D006886
1768 19901-19904 Chemical denotes HCQ MESH:D006886
1769 19922-19934 Chemical denotes pioglitazone MESH:D000077205
1770 20125-20132 Chemical denotes glucose MESH:D005947
1771 20241-20252 Chemical denotes cholesterol MESH:D002784
1772 20289-20292 Chemical denotes HCQ MESH:D006886
1773 20298-20310 Chemical denotes pioglitazone MESH:D000077205
1774 20358-20361 Chemical denotes HCQ MESH:D006886
1775 17989-17997 Disease denotes diabetic MESH:D003920
1776 18049-18080 Disease denotes glucose and insulin homeostasis MESH:D044882
1777 18166-18174 Disease denotes diabetic MESH:D003920
1778 18457-18465 Disease denotes diabetic MESH:D003920
1779 18594-18602 Disease denotes diabetic MESH:D003920
1780 18691-18699 Disease denotes diabetic MESH:D003920
1781 18774-18780 Disease denotes stress MESH:D000079225
1782 19038-19052 Disease denotes diabetic obese MESH:D003920
1783 19272-19290 Disease denotes obese non-diabetic MESH:D003920
1784 19789-19797 Disease denotes diabetes MESH:D003920
1785 19858-19866 Disease denotes diabetic MESH:D003920
1786 19950-19958 Disease denotes diabetic MESH:D003920
1787 20404-20412 Disease denotes diabetes MESH:D003920
1791 20447-20453 Disease denotes Cancer MESH:D009369
1792 20455-20467 Disease denotes Inflammation MESH:D007249
1793 20469-20492 Disease denotes Cardiovascular Diseases MESH:D002318
1813 20953-20957 Species denotes mice Tax:10090
1814 20534-20537 Chemical denotes HCQ MESH:D006886
1815 20764-20767 Chemical denotes HCQ MESH:D006886
1816 20971-20983 Chemical denotes azoxymethane MESH:D001397
1817 20988-21010 Chemical denotes dextran sodium sulfate
1818 21094-21097 Chemical denotes HCQ MESH:D006886
1819 21251-21254 Chemical denotes HCQ MESH:D006886
1820 21466-21469 Chemical denotes ROS MESH:D017382
1821 21543-21546 Chemical denotes HCQ MESH:D006886
1822 20546-20558 Disease denotes inflammation MESH:D007249
1823 20640-20646 Disease denotes cancer MESH:D009369
1824 20658-20689 Disease denotes Chronic intestinal inflammation MESH:D007249
1825 20717-20753 Disease denotes colitis-associated colorectal cancer MESH:D015179
1826 20803-20809 Disease denotes cancer MESH:D009369
1827 20918-20923 Disease denotes tumor MESH:D009369
1828 21021-21027 Disease denotes cancer MESH:D009369
1829 21217-21222 Disease denotes tumor MESH:D009369
1830 21381-21386 Disease denotes tumor MESH:D009369
1831 21411-21423 Disease denotes inflammation MESH:D007249
1878 21793-21801 Species denotes patients Tax:9606
1879 21842-21845 Species denotes rat Tax:10116
1880 22364-22367 Species denotes rat Tax:10116
1881 22805-22809 Species denotes rats Tax:10116
1882 22960-22964 Species denotes mice Tax:10090
1883 23376-23381 Species denotes mouse Tax:10090
1884 23940-23944 Species denotes rats Tax:10116
1885 24332-24337 Species denotes mouse Tax:10090
1886 21750-21753 Chemical denotes HCQ MESH:D006886
1887 21826-21829 Chemical denotes HCQ MESH:D006886
1888 22071-22074 Chemical denotes HCQ MESH:D006886
1889 22199-22202 Chemical denotes HCQ MESH:D006886
1890 22563-22569 Chemical denotes lipids MESH:D008055
1891 22712-22715 Chemical denotes HCQ MESH:D006886
1892 22731-22742 Chemical denotes fatty acids MESH:D005227
1893 22744-22757 Chemical denotes triglycerides MESH:D014280
1894 22765-22776 Chemical denotes cholesterol MESH:D002784
1895 22856-22859 Chemical denotes HCQ MESH:D006886
1896 23255-23258 Chemical denotes HCQ MESH:D006886
1897 23405-23408 Chemical denotes HCQ MESH:D006886
1898 23748-23751 Chemical denotes HCQ MESH:D006886
1899 24007-24010 Chemical denotes HCQ MESH:D006886
1900 24176-24179 Chemical denotes HCQ MESH:D006886
1901 24368-24371 Chemical denotes HCQ MESH:D006886
1902 24650-24653 Chemical denotes HCQ MESH:D006886
1903 21994-22002 Disease denotes ischemia MESH:D007511
1904 22119-22146 Disease denotes ischemia-reperfusion injury MESH:D015427
1905 22224-22239 Disease denotes cardiac infarct MESH:D006331
1906 22346-22351 Disease denotes death MESH:D003643
1907 22388-22403 Disease denotes atherosclerotic MESH:D050197
1908 22450-22463 Disease denotes heart failure MESH:D006333
1909 22605-22620 Disease denotes atherosclerotic MESH:D050197
1910 22678-22684 Disease denotes stress MESH:D000079225
1911 22690-22710 Disease denotes platelet aggregation MESH:D001791
1912 22796-22804 Disease denotes diabetic MESH:D003920
1913 22978-22993 Disease denotes atherosclerotic MESH:D050197
1914 23185-23215 Disease denotes gastrointestinal inflammations MESH:D005767
1915 23227-23253 Disease denotes inflammatory bowel disease MESH:D015212
1916 23392-23399 Disease denotes colitis MESH:D003092
1917 23627-23639 Disease denotes Inflammation MESH:D007249
1918 23709-23731 Disease denotes pulmonary hypertension MESH:D006976
1919 23912-23935 Disease denotes ventricular hypertrophy MESH:D002312
1920 23950-23972 Disease denotes pulmonary hypertension MESH:D006976
1921 24043-24056 Disease denotes endometriosis MESH:D004715
1922 24348-24361 Disease denotes endometriosis MESH:D004715
1923 24513-24538 Disease denotes impairment of the disease MESH:D060825

LitCovid-PD-HP

Id Subject Object Predicate Lexical cue hp_id
T55 292-312 Phenotype denotes auto-immune diseases http://purl.obolibrary.org/obo/HP_0002960
T56 319-339 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T57 513-531 Phenotype denotes autoimmune disease http://purl.obolibrary.org/obo/HP_0002960
T58 637-650 Phenotype denotes hyperglycemia http://purl.obolibrary.org/obo/HP_0003074
T59 652-666 Phenotype denotes hyperlipidemia http://purl.obolibrary.org/obo/HP_0003077
T60 1569-1589 Phenotype denotes Rheumatoid Arthritis http://purl.obolibrary.org/obo/HP_0001370
T61 1590-1610 Phenotype denotes Rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T62 1625-1643 Phenotype denotes autoimmune disease http://purl.obolibrary.org/obo/HP_0002960
T63 1709-1729 Phenotype denotes Immune dysregulation http://purl.obolibrary.org/obo/HP_0002958
T64 1760-1780 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T65 1979-1999 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T66 2127-2140 Phenotype denotes hyperactivity http://purl.obolibrary.org/obo/HP_0000752
T67 2439-2448 Phenotype denotes arthritis http://purl.obolibrary.org/obo/HP_0001369
T68 2850-2870 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T69 2988-2997 Phenotype denotes synovitis http://purl.obolibrary.org/obo/HP_0100769
T70 3002-3012 Phenotype denotes joint pain http://purl.obolibrary.org/obo/HP_0002829
T71 3672-3676 Phenotype denotes pain http://purl.obolibrary.org/obo/HP_0012531
T72 3923-3943 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T73 4155-4167 Phenotype denotes hypertension http://purl.obolibrary.org/obo/HP_0000822
T74 4169-4176 Phenotype denotes obesity http://purl.obolibrary.org/obo/HP_0001513
T75 4569-4581 Phenotype denotes dyslipidemia http://purl.obolibrary.org/obo/HP_0003119
T76 4701-4721 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T77 5109-5129 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T78 5272-5292 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T79 5577-5597 Phenotype denotes rheumatoid arthritis http://purl.obolibrary.org/obo/HP_0001370
T80 5693-5711 Phenotype denotes insulin resistance http://purl.obolibrary.org/obo/HP_0000855
T81 6050-6059 Phenotype denotes arthritis http://purl.obolibrary.org/obo/HP_0001369
T82 6125-6153 Phenotype denotes Systemic lupus erythematosus http://purl.obolibrary.org/obo/HP_0002725
T83 7110-7133 Phenotype denotes constitutional symptoms http://purl.obolibrary.org/obo/HP_0025142
T84 7174-7183 Phenotype denotes arthritis http://purl.obolibrary.org/obo/HP_0001369
T85 8335-8354 Phenotype denotes autoimmune diseases http://purl.obolibrary.org/obo/HP_0002960
T86 9155-9174 Phenotype denotes kidney inflammation http://purl.obolibrary.org/obo/HP_0000123
T87 10925-10948 Phenotype denotes endothelial dysfunction http://purl.obolibrary.org/obo/HP_0032654
T88 10973-10995 Phenotype denotes cardiovascular disease http://purl.obolibrary.org/obo/HP_0001626
T89 11008-11020 Phenotype denotes hypertension http://purl.obolibrary.org/obo/HP_0000822
T90 11146-11167 Phenotype denotes thromboembolic events http://purl.obolibrary.org/obo/HP_0001907
T91 11195-11207 Phenotype denotes hypertension http://purl.obolibrary.org/obo/HP_0000822
T92 11602-11625 Phenotype denotes endothelial dysfunction http://purl.obolibrary.org/obo/HP_0032654
T93 11648-11663 Phenotype denotes atherosclerosis http://purl.obolibrary.org/obo/HP_0002621
T94 13438-13447 Phenotype denotes nephritis http://purl.obolibrary.org/obo/HP_0000123
T95 13532-13557 Phenotype denotes small for gestational age http://purl.obolibrary.org/obo/HP_0001518
T96 13715-13734 Phenotype denotes autoimmune disorder http://purl.obolibrary.org/obo/HP_0002960
T97 13831-13850 Phenotype denotes autoimmune diseases http://purl.obolibrary.org/obo/HP_0002960
T98 14679-14694 Phenotype denotes thromboembolism http://purl.obolibrary.org/obo/HP_0001907
T99 15809-15827 Phenotype denotes autoimmune disease http://purl.obolibrary.org/obo/HP_0002960
T100 16013-16023 Phenotype denotes xerostomia http://purl.obolibrary.org/obo/HP_0000217
T101 18669-18699 Phenotype denotes insulin resistance in diabetic http://purl.obolibrary.org/obo/HP_0000831
T102 19414-19432 Phenotype denotes insulin resistance http://purl.obolibrary.org/obo/HP_0000855
T103 20447-20453 Phenotype denotes Cancer http://purl.obolibrary.org/obo/HP_0002664
T104 20469-20492 Phenotype denotes Cardiovascular Diseases http://purl.obolibrary.org/obo/HP_0001626
T105 20640-20646 Phenotype denotes cancer http://purl.obolibrary.org/obo/HP_0002664
T106 20717-20724 Phenotype denotes colitis http://purl.obolibrary.org/obo/HP_0002583
T107 20747-20753 Phenotype denotes cancer http://purl.obolibrary.org/obo/HP_0002664
T108 20803-20809 Phenotype denotes cancer http://purl.obolibrary.org/obo/HP_0002664
T109 20918-20923 Phenotype denotes tumor http://purl.obolibrary.org/obo/HP_0002664
T110 21021-21027 Phenotype denotes cancer http://purl.obolibrary.org/obo/HP_0002664
T111 21217-21222 Phenotype denotes tumor http://purl.obolibrary.org/obo/HP_0002664
T112 21381-21386 Phenotype denotes tumor http://purl.obolibrary.org/obo/HP_0002664
T113 22450-22463 Phenotype denotes heart failure http://purl.obolibrary.org/obo/HP_0001635
T114 23185-23215 Phenotype denotes gastrointestinal inflammations http://purl.obolibrary.org/obo/HP_0004386
T115 23227-23253 Phenotype denotes inflammatory bowel disease http://purl.obolibrary.org/obo/HP_0002037
T116 23392-23399 Phenotype denotes colitis http://purl.obolibrary.org/obo/HP_0002583
T117 23719-23731 Phenotype denotes hypertension http://purl.obolibrary.org/obo/HP_0000822
T118 23912-23935 Phenotype denotes ventricular hypertrophy http://purl.obolibrary.org/obo/HP_0001714
T119 23960-23972 Phenotype denotes hypertension http://purl.obolibrary.org/obo/HP_0000822
T120 24043-24056 Phenotype denotes endometriosis http://purl.obolibrary.org/obo/HP_0030127
T121 24348-24361 Phenotype denotes endometriosis http://purl.obolibrary.org/obo/HP_0030127

LitCovid-sentences

Id Subject Object Predicate Lexical cue
T266 0-4 Sentence denotes 2.3.
T267 5-43 Sentence denotes Hydroxychloroquine Biological Activity
T268 44-149 Sentence denotes Besides the antiviral effects, HCQ possesses several other demonstrated biological activities (Figure 6).
T269 150-421 Sentence denotes Most of all, it showed immunosuppressive properties, allowing its employment (alone or in combination) in the first-line treatment of several auto-immune diseases, like rheumatoid arthritis, lupus erythematosus, primary Sjögren’s syndrome, and anti-phospholipid syndrome.
T270 422-700 Sentence denotes Moreover, HCQ was revealed to be effective in preclinical and clinical trials to dampening autoimmune disease-dependent cardiovascular complications (Figure 7), as well as in the amelioration of disease-independent hyperglycemia, hyperlipidemia, and gastrointestinal complaints.
T271 701-789 Sentence denotes HCQ exerts anticancer effects by acting synergistically with common chemotherapic drugs.
T272 790-987 Sentence denotes Although it has a well-defined and favorable toxicity profile, the necessity of increasing the dose, in some cases, limits the utilization, due to the toxicity, mainly at cardiac and ocular levels.
T273 988-1095 Sentence denotes A two-compartment model, with first-order absorption and a lag time, describes the pharmacokinetics of HCQ.
T274 1096-1216 Sentence denotes The long-terminal half-life prolongs the time to reach steady-state concentrations, then delays the therapeutic effects.
T275 1217-1295 Sentence denotes The next-generation formulations allow modulating the pharmacokinetics of HCQ.
T276 1296-1435 Sentence denotes Avoiding systemic absorption, then liver first-pass metabolism, HCQ may be used in site-specific inflammation, without toxicity [72,73,74].
T277 1436-1560 Sentence denotes The selected studies’ primary outcomes are the extent to which HCQ may limit disease progression or exacerbations (Table 2).
T278 1562-1568 Sentence denotes 2.3.1.
T279 1569-1589 Sentence denotes Rheumatoid Arthritis
T280 1590-1708 Sentence denotes Rheumatoid arthritis is a systemic autoimmune disease, characterized by chronic inflammation and damage to the joints.
T281 1709-1939 Sentence denotes Immune dysregulation underlies the pathogenesis of rheumatoid arthritis, leading to uncontrolled production of antibodies, mainly rheumatoid factor and citrullinate, involved in the autoreactivity against cartilage and bone [117].
T282 1940-2036 Sentence denotes It is estimated that the prevalence of rheumatoid arthritis is around 1%, mainly in women [118].
T283 2037-2212 Sentence denotes The immunosuppressive effects of HCQ are due to the ability to modulate T-cell and B-cell hyperactivity, resulting in a reduction of pro-inflammatory cytokine gene expression.
T284 2213-2449 Sentence denotes As the involvement of neutrophils in this disease, Jancinova, Pazourekova, Lucova, Perecko, Mihalova, Bauerova, Nosal and Drabikova [75] investigated the impact of oral HCQ administration on these cells, in rats with adjuvant arthritis.
T285 2450-2661 Sentence denotes At doses of 40 mg/kg daily, per oral administration (p.o.), it strongly decreased the blood concentration of neutrophil-derived oxidants, involved in the tissue damage and the onset of chronic inflammation [75].
T286 2662-2871 Sentence denotes A 36-week randomized, double-blind, placebo-controlled trial has evaluated the effect of the administration of HCQ in a dose of up to 7 mg/kg per day (maximum 400 mg/day) in patients with rheumatoid arthritis.
T287 2872-3063 Sentence denotes Within 36 weeks and during the study, HCQ showed statistically significant benefits on physical function, mainly on synovitis and joint pain, without side effects with respect to the control.
T288 3064-3139 Sentence denotes Moreover, HCQ was associated with a decrement of corticosteroid injections.
T289 3140-3223 Sentence denotes By contrast, no improvements in psychological function have been demonstrated [76].
T290 3224-3474 Sentence denotes Two comparative double-blind, randomized trials, involving 60 patients each, with sulfasalazine and HCQ have demonstrated that HCQ showed no significant differences among overall clinical effects respect to sulfasalazine, but presented a later onset.
T291 3475-3905 Sentence denotes In the first study, patients treated with HCQ (400 mg/day for 6 months and 200 mg/day for the next 6 months) experienced time-dependent statistically significant improvements in morning stiffness, pain, swollen joints, together with a decrease in blood levels of immunoglobulin M and erythrocyte sedimentation rate [77], while, in the second study, the same treatment was associated to no erosions in the 12% of the patients [78].
T292 3906-4026 Sentence denotes In patients with rheumatoid arthritis, the cardiovascular risk is more than doubled, compared to the healthy population.
T293 4027-4201 Sentence denotes Chronic inflammatory status leads to an intensification of the atherosclerotic process, resulting in a higher susceptibility to hypertension, obesity, and metabolic syndrome.
T294 4202-4322 Sentence denotes The overproduction of IL-6 is strictly related to lipid profile alterations, given its role in adipose tissue lipolysis.
T295 4323-4400 Sentence denotes The inflammation and endothelial damage are exacerbated by leptin production.
T296 4401-4538 Sentence denotes Batun-Garrido, Salas-Magana and Juarez-Rojop [79] found a significant correlation between HCQ treatment and lower IL-6 and leptin levels.
T297 4539-4904 Sentence denotes The positive effect of HCQ on dyslipidemia was also confirmed by Morris, Wasko, Antohe, Sartorius, Kirchner, Dancea and Bili [80] in a cohort study involving 706 rheumatoid arthritis diagnosed patients, finding a significant and stable cholesterol-lowering, mainly Low-Density Lipoprotein (LDL), and triglyceride decrease associated with HCQ intake (6.5 mg/kg/day).
T298 4905-5135 Sentence denotes A small but statistically significant amelioration in total cholesterol and LDL under HCQ treatment at the same dosage was also highlighted by a randomized, double-blind cross-over trial on patients with rheumatoid arthritis [81].
T299 5136-5293 Sentence denotes The correlation between HCQ and cardiovascular risk was also assessed in a cross-sectional observational study involving 177 women with rheumatoid arthritis.
T300 5294-5430 Sentence denotes At doses of 200 mg/kg/day, HCQ usage led to lower fasting glucose in women, arising as a valuable tool to enhance glycemic control [82].
T301 5431-5646 Sentence denotes However, apparent different outcomes were derived from a randomized double-blind crossover trial, recruiting 23 non-diabetic subjects with stable rheumatoid arthritis to receive 6.5 mg/kg/day of HCQ for eight weeks.
T302 5647-5733 Sentence denotes For these patients, no significant changes in insulin resistance were observable [81].
T303 5734-5866 Sentence denotes This study evaluated only insulin sensitivity, by Homeostatic Model Assessment (HOMA) index, without considering insulin metabolism.
T304 5867-5969 Sentence denotes Thus, inconsistency should be explained by this factor, together with the short duration of treatment.
T305 5970-6096 Sentence denotes The anti-diabetic properties of HCQ have been also assessed in patients without arthritis, as reported in the next paragraphs.
T306 6098-6104 Sentence denotes 2.3.2.
T307 6105-6124 Sentence denotes Lupus Erythematosus
T308 6125-6287 Sentence denotes Systemic lupus erythematosus is a multisystemic autoimmune chronic inflammatory disorder that mainly involves joints, mucosae, skin, and endothelial vessels [90].
T309 6288-6377 Sentence denotes For a long time, HCQ has played a marginal role in the overall management of the disease.
T310 6378-6533 Sentence denotes Since the 90s, the first evidence of HCQ effectiveness in controlling lupus erythematosus manifestations allowed its employment as a first-line medicament.
T311 6534-6683 Sentence denotes Although it was not recommended in single therapy, the immunomodulating properties of HCQ seem to play an important role in the disease pathogenesis.
T312 6684-6816 Sentence denotes It is associated with a decrement of exacerbation events, as well as protective effects towards vascular and thrombotic events [85].
T313 6817-7064 Sentence denotes Indeed, a 24-week randomized, double-blind placebo-controlled trial demonstrated that the discontinuing of HCQ treatment (100–400 mg/kg/day for at least six months) increased the risk of exacerbations by 2.5 times in patients with quiescent lupus.
T314 7065-7201 Sentence denotes People who interrupted the therapy exhibited constitutional symptoms of the disease, as well as skin rashes, arthritis, and ulcers [83].
T315 7202-7417 Sentence denotes A long-term randomized study evaluated the withdrawal effects of HCQ on quiescent lupus erythematosus patients, revealing that a reduction by up to 57% is associated with HCQ maintaining treatment (272 mg/day) [84].
T316 7418-7539 Sentence denotes A case-control study was carried out in order to define the role of HCQ in the survival of individuals affected by lupus.
T317 7540-7717 Sentence denotes The positive correlation between HCQ and survival led to the consideration of this drug as a great therapeutic option at the proper dose (6.5 mg/kg/bw) in lupus management [85].
T318 7718-7947 Sentence denotes If these clinical trials demonstrated the advantages of keeping up the therapy with HCQ in preventing disease exacerbations, doubts persisted about the efficacy of this treatment in the control of more severe clinical forms [83].
T319 7948-8122 Sentence denotes As the important role of the imbalance between immune cell populations, several preclinical and clinical studies have evaluated the role of HCQ in restoring this equilibrium.
T320 8123-8379 Sentence denotes In particular, elevated levels of effector lymphocyte T (Th17) that mediate the autoimmune answer and decreased levels of regulatory lymphocyte T (Treg) that guarantees the immune homeostasis, may be observed in autoimmune diseases, in particular in lupus.
T321 8380-8472 Sentence denotes Lately, autophagy had risen among the emerging strategies to reestablish the immune balance.
T322 8473-8634 Sentence denotes As HCQ is a well-known autophagy inhibitor, An, N. et al. [86] evaluated the influence of HCQ intake (100 mg/kg/day) in MRL/lpr mice with the lupus-like disease.
T323 8635-8785 Sentence denotes After four weeks of treatment, HCQ clearly restored the immune balance, by both inhibiting Th17 response and enhancing Treg immunosuppressive effects.
T324 8786-9068 Sentence denotes The levels of autoantibodies and the expression of inflammatory cytokines, mainly in Th17 cells, were remarkably lowered, due to the inhibition of the activated autophagy, as demonstrated by the increase of autophagic flux marker expression in Th17 and Treg, compared with controls.
T325 9069-9253 Sentence denotes This randomized trial further evidenced that HCQ treatment also remarkably attenuated kidney inflammation, by limiting the migration of lymphoplasmacytic cells into renal tissues [86].
T326 9254-9405 Sentence denotes Preclinical outcomes have been confirmed by a prospective cohort study, involving 41 patients with a diagnosis of lupus treated with 400 mg/day of HCQ.
T327 9406-9756 Sentence denotes Dysregulated cytokine and autoantibody production, deriving from high autoreactivity that characterizes lupus disease, has been restored by two months of HCQ administration, demonstrating its ability in modulating inflammatory response, with normalized complement activity and reduced levels of pro-inflammatory cytokines, mainly IL-6 and TNF-α [87].
T328 9757-10049 Sentence denotes In a multiethnic US cohort on 35 lupus patients, HCQ treatment resulted in significant clinical benefits towards disease progression, probably due to the inhibition of toll-like receptor activation, resulting in down-regulation of IFN-α, which plays a pivotal role in lupus pathogenesis [88].
T329 10050-10181 Sentence denotes Infiltrating cells, most of all mast cells, could involve skin tissues, causing one of the most common signs of lupus, skin rashes.
T330 10182-10343 Sentence denotes The consequences of HCQ intake on skin lesions have been investigated on a MRL/lpr murine model of lupus at low (4 mg/kg/day) and high (40 mg/kg/day) oral doses.
T331 10344-10578 Sentence denotes The number of mast cells decreased with respect to the drinking-water control (from 81 to 50 in low-dose and 12 in high dose), while the mortality rate decreased by up to three times in both treated groups with respect to the control.
T332 10579-10751 Sentence denotes These in vivo results, together with a significant histopathological alteration regression, suggest that HCQ is a good tool against skin injury in lupus erythematosus [89].
T333 10752-10883 Sentence denotes The chronic inflammatory status that features lupus erythematosus leads to a higher susceptibility to cardiovascular complications.
T334 10884-11038 Sentence denotes Lupus, indeed, is often characterized by endothelial dysfunction, the earliest marker of cardiovascular disease, as well as hypertension and renal damage.
T335 11039-11168 Sentence denotes In a NZB/W F1 mice model of lupus, oral HCQ gavage of 10 mg/kg/day for five weeks reduced the incidence of thromboembolic events.
T336 11169-11386 Sentence denotes Moreover, improvements in hypertension, renal damage, and heart hypertrophy occurred, probably due to the normalized endothelium response and reduction of Reactive Oxygen Species (ROS) attributable to HCQ intake [90].
T337 11387-11516 Sentence denotes The same effect of normalizing nitric oxide and ROS production have been confirmed in a NZB/W F1 murine model at different times.
T338 11517-11631 Sentence denotes HCQ at 3 mg/kg/day p.o. protected vascular endothelium, with a strong improvement of endothelial dysfunction [91].
T339 11632-11714 Sentence denotes The benefits on atherosclerosis also pass through the lipid-lowering power of HCQ.
T340 11715-11941 Sentence denotes A clinical study on 155 autoimmune patients revealed a statistically significant association between HCQ (400 mg/day) and a lessening of triglyceride and cholesterol levels, mainly LDL, while no HDL changes were observed [92].
T341 11942-12049 Sentence denotes By contrast, HCQ in patients with a mild or inactive condition had no significant effects on lipid profile.
T342 12050-12277 Sentence denotes A survey involving 65 Chinese lupus patients, treated with HCQ (244 ± 86 mg/day), demonstrated that only triglycerides tended to be lowered, while no statistically significant changes are observable in cholesterol levels [119].
T343 12278-12394 Sentence denotes The use of HCQ may be helpful in minimizing cardiovascular risk by improving glycemic homeostasis in lupus patients.
T344 12395-12648 Sentence denotes A cross-sectional study performed between 2000 and 2005 on 149 nondiabetic women affected by lupus estimated that a mean dose of 400 mg of HCQ affects insulin sensitivity and resistance, as assessed by HOMA index, as well as fasting glucose levels [82].
T345 12649-12790 Sentence denotes HCQ remains a worthwhile primary or additional therapy in lupus patients, considering the low cost and its safety profile, also in pregnancy.
T346 12791-12962 Sentence denotes A randomized double-blind study reported the safety of HCQ during pregnancy, correlating this drug with less disease activity and a lower required dose of prednisone [93].
T347 12963-13073 Sentence denotes A 5-year prospective study evaluated the effect of HCQ discontinuation on lupus progression in pregnant women.
T348 13074-13184 Sentence denotes As it occurs in no pregnant people, interruption of HCQ treatment is linked to an exacerbation of the disease.
T349 13185-13381 Sentence denotes Moreover, there are no statistically significant differences regarding pregnant complications with respect to the control, showing no fetal toxicity at a dose of 6.5 mg/kg/day in breast milk [94].
T350 13382-13585 Sentence denotes Fetal safety has been also assessed in women with lupus nephritis by a multicenter study, reporting a reduction of 85% of the possibility of having a small for gestational age baby in patients under HCQ.
T351 13586-13648 Sentence denotes Moreover, it exerted protective effects on fetal growth [120].
T352 13650-13656 Sentence denotes 2.3.3.
T353 13657-13682 Sentence denotes Antiphospholipid Syndrome
T354 13683-13795 Sentence denotes Antiphospholipid syndrome is an autoimmune disorder characterized by antiphospholipid autoantibodies production.
T355 13796-13878 Sentence denotes If it is not associated with other autoimmune diseases, it is called primary [97].
T356 13879-14088 Sentence denotes The incidence of the pathology is greater in young women of reproductive age and it often has a negative impact on pregnancy, with unfortunate outcomes due to the development of placental ischemic pathologies.
T357 14089-14221 Sentence denotes Resonance spectroscopy, indeed, revealed that the fetal brain and placenta are the main targets of autoantibodies localization [95].
T358 14222-14382 Sentence denotes As complement activation plays a central role in the occurrence of the disease, many studies have evaluated the role of HCQ in inhibiting complement activation.
T359 14383-14604 Sentence denotes In a mouse model of obstetric antiphospholipid syndrome, HCQ, administered in a daily dose of 200 μg per mouse limited placental abnormalities, with an increase of fetal survival, by inhibiting complement activation [95].
T360 14605-14751 Sentence denotes A case report on the use of HCQ on a pregnant woman with recurrent venous thromboembolism confirmed the efficacy of HCQ also in clinical practice.
T361 14752-14946 Sentence denotes The addition of 400 mg daily of HCQ to a common therapeutic regimen of aspirin and heparin dramatically reduced the episodes of vascular thrombosis [96], showing great antithrombotic properties.
T362 14947-15045 Sentence denotes Given these results, the mechanisms underlying the use of HCQ in thromboprophylaxis were assessed.
T363 15046-15427 Sentence denotes Two similar preclinical studies, using one-week treatment with 12 μg/g/day of HCQ and three-weeks treatment with 20 mg/kg/day of HCQ, respectively, were in accordance to assess that the overall amelioration of thrombotic status in mice models of antiphospholipid syndrome was linked to endothelial function improvement by modulating the expression of nitric oxide synthase [97,98].
T364 15428-15539 Sentence denotes Moreover, the efficacy of HCQ in antithrombotic therapy may lie in the interference in the coagulation cascade.
T365 15540-15760 Sentence denotes HCQ, indeed, was revealed to decrease the levels of soluble tissue factor, a key initiator of the process, in patients with antiphospholipid syndrome after three months of therapy with a daily dose of HCQ of 200 mg [99].
T366 15762-15768 Sentence denotes 2.3.4.
T367 15769-15785 Sentence denotes Sjögren Syndrome
T368 15786-15900 Sentence denotes Sjögren syndrome is an autoimmune disease with a strong negative impact on the quality of life of affected people.
T369 15901-16030 Sentence denotes The main features of the disease are lymphocytic inflammation and alterations in major salivary glands, causing xerostomia [103].
T370 16031-16185 Sentence denotes Even if preliminary results about HCQ use in Sjögren syndrome were not encouraging, to date it arises as one of the first-line drugs in disease treatment.
T371 16186-16476 Sentence denotes Indeed, an earlier prospective, a two-year double-blind crossover trial on 19 subjects correlated an annual intake of a dose of 400 mg/day with no significant improvements in clinical symptoms and signs of pathology, including tear and salivary gland activity, respect to the placebo [121].
T372 16477-16588 Sentence denotes However, a few years later, the first evidence of HCQ effectiveness in Sjögren syndrome treatment was reported.
T373 16589-16822 Sentence denotes Annual treatment with a dose of 200 mg/day of HCQ showed anti-lymphoproliferative and anti-inflammatory effects, with a reduction of IgG and IgA immunoglobulins, anti-Sjögren autoantibodies, and erythrocyte sedimentation rates [100].
T374 16823-17083 Sentence denotes Moreover, the salivary flow rate increased in Sjögren syndrome women who received a daily dose of 400 mg of HCQ for 30 weeks [101], while eye dryness was alleviated by HCQ administration (6.5 mg/kg), as demonstrated by a prospective study on 32 patients [102].
T375 17084-17242 Sentence denotes Hypo-salivation deriving from acinar atrophy and fibrosis of salivary glands is often associated with over-expression of TGF-β (transforming growth factor-β).
T376 17243-17465 Sentence denotes Treatment with HCQ downregulated TGF-β levels in a randomized trial on NOD mice exposed to doses of 50 mg/kg/day intragastrically (i.g.) for 16 weeks, with significant results in delaying loss of saliva secretory function.
T377 17466-17592 Sentence denotes Moreover, HCQ intake was also accompanied by a decrease in autoantibody production and a lower lymphocytic infiltration [103].
T378 17593-17885 Sentence denotes These findings were confirmed by Wu, Pu, Yu and Li [104], showing that 8-weeks treatment with HCQ administered at a dose of 60 mg/kg i.g. in 40 randomized NOD mice led to lower lymphocytic infiltration, with a significant improvement in pathological changes in submandibular gland morphology.
T379 17887-17893 Sentence denotes 2.3.5.
T380 17894-17902 Sentence denotes Diabetes
T381 17903-18009 Sentence denotes As has already been demonstrated for autoimmune patients, HCQ demonstrated great anti-diabetic properties.
T382 18010-18355 Sentence denotes The first proofs of the role of HCQ in glucose and insulin homeostasis date back to 1999, when Emami, Gerstein, Pasutto, and Jamali [105] demonstrated that diabetic rats treated with oral doses of 80, 120, and 160 mg/kg/day of HCQ exhibited a dose-dependent increase in insulin blood levels, with a consequent reduction of glucose concentration.
T383 18356-18608 Sentence denotes Higher doses of HCQ (200 mg/kg/day) were tested by Abdel-Hamid, A.A. and El-Firgany Ael, D. [106] on diabetic rats, finding an HCQ-mediated decrease in the pancreas, as the mechanism underlying the improvement of the metabolic profile in diabetic rats.
T384 18609-18795 Sentence denotes The same authors associated the beneficial impact of HCQ on insulin resistance in diabetic rats with its ability to restore adipokine balance and reduce endothelial stress markers [113].
T385 18796-18937 Sentence denotes Given the positive outcomes deriving from preclinical studies, the therapeutic potential of HCQ was also assessed in several clinical trials.
T386 18938-19062 Sentence denotes Included in a randomized, double-blinded study of 18 months with 300 mg of HCQ twice a day were 135 diabetic obese patients.
T387 19063-19226 Sentence denotes HCQ treatment improved glycemic control, as demonstrated by the decrease of glycated hemoglobin by up to 1% respect to the placebo, without any side effects [107].
T388 19227-19463 Sentence denotes An open-label longitudinal study engaging 13 obese non-diabetic individuals examined the effects of a dose of 6.5 mg/kg/day of HCQ for six weeks, demonstrating a significant reduction in insulin resistance, assessed by HOMA index [108].
T389 19464-19653 Sentence denotes In a randomized, double-blinded, controlled trial on 39 prediabetic subjects, the effect of 12-week treatment with 6.5 mg/kg/day of HCQ on glycemic status and lipidic profile was evaluated.
T390 19654-19804 Sentence denotes Results reported a significant increase in insulin levels, demonstrating the potential use of HCQ to counteract the risk of developing diabetes [109].
T391 19805-20013 Sentence denotes A randomized double-blind study involving 267 type-2 diabetic patients compared the efficacy of HCQ (400 mg/day) and pioglitazone, a common anti-diabetic drug, in the control of glycemic and lipidic profiles.
T392 20014-20208 Sentence denotes No statistically significant differences emerged between the two medicines in terms of glycated hemoglobin and glucose levels, although both drugs produced an improvement in glycemic parameters.
T393 20209-20311 Sentence denotes Regarding lipidic status, total cholesterol and LDL levels were reduced more by HCQ than pioglitazone.
T394 20312-20430 Sentence denotes Given the good tolerability of the treatment, HCQ may arise as a therapeutic alternative in diabetes management [110].
T395 20432-20438 Sentence denotes 2.3.6.
T396 20439-20493 Sentence denotes Others (Cancer, Inflammation, Cardiovascular Diseases)
T397 20494-20657 Sentence denotes Given the well-recognized properties of HCQ against inflammation, it is easily intuitable that this agent could possess interesting insights into cancer treatment.
T398 20658-20754 Sentence denotes Chronic intestinal inflammation predisposes to the risk of colitis-associated colorectal cancer.
T399 20755-21028 Sentence denotes In vivo, HCQ was demonstrated to interfere with cancer growth at different stages of development, both preventing tumorigenesis in the early phases and inhibiting tumor growth in the late phases in mice treated with azoxymethane and dextran sodium sulfate to induce cancer.
T400 21029-21223 Sentence denotes In terms of animal survival, 120 days treatment with 50 mg/kg of HCQ intraperitoneal injection (i.p.) almost restored the survival rate to pre-treatment values and reduced the size of the tumor.
T401 21224-21502 Sentence denotes The therapeutic effects of HCQ may be attributed to the significant inhibition of pro-tumorigenic and pro-inflammatory cytokines, which not only limited the tumor progression by reducing inflammation of lamina propria, but also decreased the ROS production in macrophages [111].
T402 21503-21652 Sentence denotes Many others are the mechanisms by which HCQ exerts anticancer effects, mainly in synergism with conventional chemotherapic drugs, as discussed later.
T403 21653-21802 Sentence denotes Regarding the cardioprotective effect, this review has already focused on the positive impact of HCQ on cardiovascular issues in autoimmune patients.
T404 21803-22029 Sentence denotes A protective effect of HCQ on neonatal rat cardiomyocytes was proven by Bourke, McCormick, Taylor, Pericleous, Blanchet, Costedoat-Chalumeau, Stuckey, Lythgoe, Stephanou and Ioannou [112] in ischemia-reperfusion animal models.
T405 22030-22147 Sentence denotes The pharmacological preconditioning with HCQ seems to be a good strategy to protect from ischemia-reperfusion injury.
T406 22148-22252 Sentence denotes The pretreatment with daily gavage of 200 mg/kg of HCQ, indeed, reduced the cardiac infarct size by 47%.
T407 22253-22383 Sentence denotes The mechanism underlying this effect is linked to the inhibition of apoptosis and total cell death in neonatal rat cardiomyocytes.
T408 22384-22464 Sentence denotes The atherosclerotic process contributes to increasing the risk of heart failure.
T409 22465-22515 Sentence denotes The etiology of this condition is still not clear.
T410 22516-22711 Sentence denotes A hypothesis supposes that the accumulation of lipids in vessels caused the formation of atherosclerotic plaques that are responsible for vessel narrowing, shear stress, and platelet aggregation.
T411 22712-22845 Sentence denotes HCQ decreased free-fatty acids, triglycerides, total cholesterol, and LDL levels in diabetic rats under doses of 200 mg/kg/day [106].
T412 22846-23040 Sentence denotes Moreover, HCQ (10 mg/kg/day) was demonstrated to exhibit functional and structural protection in 40 high-fat diet mice, by reducing atherosclerotic area by 60% with respect to the control [114].
T413 23041-23181 Sentence denotes These favorable effects at the metabolic level might be due to its anti-inflammatory power that influences many other biological activities.
T414 23182-23372 Sentence denotes In gastrointestinal inflammations, mainly in inflammatory bowel disease, HCQ suppressed pro-inflammatory cytokines and enhanced the expression of ILs involved in anti-inflammatory processes.
T415 23373-23626 Sentence denotes In mouse models of colitis, the HCQ methacryloylated form (30 mg/kg) avoided systemic absorption, accumulating in the gastrointestinal tract, where alterations in the immune homeostasis of the intestinal mucosa had a positive impact on the disease [74].
T416 23627-23732 Sentence denotes Inflammation, together with alterations in the immune system, are at the basis of pulmonary hypertension.
T417 23733-24029 Sentence denotes The ability of HCQ to interfere with the production of pro-inflammatory cytokines from monocytes and lymphocytes might underlie the observed improvements in systolic pressure and ventricular hypertrophy, in rats with pulmonary hypertension treated with 50 mg/kg/day i.p. of HCQ for 20 days [115].
T418 24030-24193 Sentence denotes Likewise, in endometriosis, the abnormal presence of endometrium in other organs leads to a chronic inflammatory status that could be affected by HCQ intervention.
T419 24194-24388 Sentence denotes Ruiz, Rockfield, Taran, Haller, Engelman, Flores, Panina-Bordignon and Nanjundan [116] observed an increment of peritoneal macrophages in mouse models of endometriosis under HCQ (60 mg/kg i.p.).
T420 24389-24539 Sentence denotes In their role of scavengers, abnormalities in these cell populations may lead to an accumulation of endometrial cells, with impairment of the disease.
T421 24540-24710 Sentence denotes Moreover, histopathologic improvement of lesions was observed, probably due to the inhibition of autophagy by HCQ that alters anoikis response of endometrial cells [116].