SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2610408002> ?p ?o ?g. }

Showing items 1 to 100 of ±148 with 100 items per page.

W2610408002 endingPage "639" @default.
W2610408002 startingPage "629" @default.
W2610408002 abstract "Summary Micro‐albuminuria and glomerular hyperfiltration are primary indicators of renal dysfunctions in Sickle Cell Disease ( SCD ), with more severe manifestations previously associated with variants in APOL 1 and HMOX 1 among African Americans. We have investigated 413 SCD patients from Cameroon. Anthropometric variables, haematological indices, crude albuminuria, albumin‐to‐creatinine ratio ( ACR ) and estimated glomerular filtration rate ( eGFR ) were measured. Patients were genotyped for 3·7 kb alpha‐globin gene ( HBA 1/ HBA 2 ) deletion, and for variants in APOL 1 (G1/G2; rs60910145, rs73885319, rs71785313) and HMOX 1 (rs3074372, rs743811). The median age was 15 years; the majority presented with micro‐albuminuria (60·9%; n = 248), and approximately half with glomerular hyperfiltration (49·5%; n = 200). Age, male sex, haemoglobin level, leucocyte count, mean corpuscular volume, blood pressure, body mass index and creatinine levels significantly affected albuminuria and/or eGFR . Co‐inheritance of alpha‐thalassaemia was protective against macro‐albuminuria ( P = 0·03). APOL 1 G1/G2 risk variants were significantly associated with the ACR ( P = 0·01) and borderline with eGFR ( P = 0·07). HMOX 1 ‐ rs743811 was borderline associated with micro‐albuminuria ( P = 0·07) and macro‐albuminuria ( P = 0·06). The results revealed a high proportion of micro‐albuminuria and glomerular hyperfiltration among Cameroonian SCD patients, and support the possible use of targeted genetic biomarkers for risks assessment." @default.
W2610408002 created "2017-05-12" @default.
W2610408002 creator A5016936793 @default.
W2610408002 creator A5023130040 @default.
W2610408002 creator A5025856031 @default.
W2610408002 creator A5050201122 @default.
W2610408002 creator A5057943240 @default.
W2610408002 creator A5061296288 @default.
W2610408002 creator A5072475306 @default.
W2610408002 date "2017-05-03" @default.
W2610408002 modified "2023-10-05" @default.
W2610408002 title "Clinical and genetic predictors of renal dysfunctions in sickle cell anaemia in Cameroon" @default.
W2610408002 cites W1467077353 @default.
W2610408002 cites W1499224629 @default.
W2610408002 cites W1527494204 @default.
W2610408002 cites W1538711197 @default.
W2610408002 cites W1550111394 @default.
W2610408002 cites W1956685882 @default.
W2610408002 cites W1967258381 @default.
W2610408002 cites W1969724251 @default.
W2610408002 cites W1974112501 @default.
W2610408002 cites W1975843987 @default.
W2610408002 cites W1978464782 @default.
W2610408002 cites W1984262249 @default.
W2610408002 cites W1987371443 @default.
W2610408002 cites W1989802873 @default.
W2610408002 cites W2007367780 @default.
W2610408002 cites W2015051012 @default.
W2610408002 cites W2017380415 @default.
W2610408002 cites W2021707555 @default.
W2610408002 cites W2026008143 @default.
W2610408002 cites W2028778467 @default.
W2610408002 cites W2030803259 @default.
W2610408002 cites W2044430482 @default.
W2610408002 cites W2045767836 @default.
W2610408002 cites W2050717506 @default.
W2610408002 cites W2052863182 @default.
W2610408002 cites W2053495832 @default.
W2610408002 cites W2054164315 @default.
W2610408002 cites W2054735613 @default.
W2610408002 cites W2055864845 @default.
W2610408002 cites W2057842953 @default.
W2610408002 cites W2059228501 @default.
W2610408002 cites W2059565705 @default.
W2610408002 cites W2067818042 @default.
W2610408002 cites W2067847104 @default.
W2610408002 cites W2068833289 @default.
W2610408002 cites W2073921582 @default.
W2610408002 cites W2075252647 @default.
W2610408002 cites W2084591996 @default.
W2610408002 cites W2085472098 @default.
W2610408002 cites W2087355617 @default.
W2610408002 cites W2098095265 @default.
W2610408002 cites W2099688189 @default.
W2610408002 cites W2101679774 @default.
W2610408002 cites W2107642100 @default.
W2610408002 cites W2115657655 @default.
W2610408002 cites W2115855925 @default.
W2610408002 cites W2116051995 @default.
W2610408002 cites W2122855609 @default.
W2610408002 cites W2124641083 @default.
W2610408002 cites W2125290890 @default.
W2610408002 cites W2133275623 @default.
W2610408002 cites W2137096226 @default.
W2610408002 cites W2144379673 @default.
W2610408002 cites W2146999612 @default.
W2610408002 cites W2147182596 @default.
W2610408002 cites W2155965977 @default.
W2610408002 cites W2163381248 @default.
W2610408002 cites W2172095904 @default.
W2610408002 cites W2252649921 @default.
W2610408002 cites W2264426339 @default.
W2610408002 cites W2308990414 @default.
W2610408002 cites W2317953783 @default.
W2610408002 cites W2334263927 @default.
W2610408002 cites W2522225801 @default.
W2610408002 cites W2529623352 @default.
W2610408002 cites W2576614944 @default.
W2610408002 cites W2607031541 @default.
W2610408002 cites W4211186710 @default.
W2610408002 cites W2005349067 @default.
W2610408002 doi "https://doi.org/10.1111/bjh.14724" @default.
W2610408002 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5660286" @default.
W2610408002 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/28466968" @default.
W2610408002 hasPublicationYear "2017" @default.
W2610408002 type Work @default.
W2610408002 sameAs 2610408002 @default.
W2610408002 citedByCount "48" @default.
W2610408002 countsByYear W26104080022017 @default.
W2610408002 countsByYear W26104080022018 @default.
W2610408002 countsByYear W26104080022019 @default.
W2610408002 countsByYear W26104080022020 @default.
W2610408002 countsByYear W26104080022021 @default.
W2610408002 countsByYear W26104080022022 @default.
W2610408002 countsByYear W26104080022023 @default.
W2610408002 crossrefType "journal-article" @default.
W2610408002 hasAuthorship W2610408002A5016936793 @default.
W2610408002 hasAuthorship W2610408002A5023130040 @default.