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1 from each patient for measurement of BLL and complete blood count.
2 (PI); 4) gingival index (GI); 5) CRP; and 6) complete blood count.
3 city was quantified via body weight loss and complete blood count.
4 d hematoanalyzer and reported as part of the complete blood count.
5 coagulation studies, serum chemistries, and complete blood counts.
6 poietic reconstitution was assessed by doing complete blood counts.
7 can be identified in individuals with normal complete blood counts.
8 t times from 4-23 days post-treatment, and a complete blood count along with blood chemistry analyses
9 e and on-treatment NLRs were calculated from complete blood counts among 60 087 participants randomiz
11 of 48 routinely obtained blood specimens for complete blood count analysis in our institutional labor
14 ngs and routine laboratory values, including complete blood count and basic metabolic panels, were no
17 imple, widely available blood tests, such as complete blood count and complete metabolic panel, could
18 ng system that utilizes routine blood tests (complete blood count and comprehensive metabolic profile
19 g a new allopurinol prescription, and QI 3 = complete blood count and creatine kinase check every 6 m
22 ucted with AP NAAT results and time-adjacent complete blood count and LFT results for adult patients
27 visits and during outpatient care, including complete blood counts and hepatic and renal function tes
28 isk of immunodeficiency had peripheral blood complete blood counts and lymphocyte subsets assayed in
30 els, hepatitis C virus (HCV) RNA levels, and complete blood counts and underwent liver biopsy at the
31 al body iron, and transferrin], hematologic (complete blood count), and inflammatory (C-reactive prot
32 to a hospital laboratory for an urinalysis, complete blood count, and a standard blood chemistry pan
33 cal parameters, including fever, heart rate, complete blood count, and bacteremia; and evaluated the
34 othrombin time, partial thromboplastin time, complete blood count, and bleeding time were recorded.
37 anoma progression with physical examination, complete blood count, and liver function tests every 3 m
38 ttery of medical tests (electrocardiography, complete blood count, and measurement of serum levels of
39 f the pulmonary circulation, pulse oximetry, complete blood count, and serum chemistries and pulmonar
40 teine (tHcy), and creatinine concentrations, complete blood count, and vitamin supplementation in 550
43 rum and pulmonary cytokines, lung histology, complete blood counts, and intestinal proliferation were
47 concentrations of ISATX247 and cyclosporine, complete blood counts, and serum chemistry profiles were
48 findings; laboratory test results, including complete blood count; and liver function test results we
49 findings; laboratory test results, including complete blood count; and liver function test results we
50 DNA level, HBsAg level, liver function test, complete blood count, aspartate aminotransferase-to-plat
51 eceived, and receipt of a bundle of 4 tests (complete blood count, basic metabolic profile, chest rad
52 k 64, changes in other PFASs, and changes in complete blood count, biochemistry, thyroid function, an
53 howed no evidence of changes in body weight, complete blood count, blood chemistry profile, cardiac c
54 ry evaluations for infection (urine culture, complete blood count, blood culture, and wound culture)
57 iodistribution of the constituent materials, complete blood counts, blood chemistry and magnetic reso
60 rmountain Risk Score (IMRS), composed of the complete blood count (CBC) and basic metabolic profile (
62 esults from a 3-year period, with associated complete blood count (CBC) and liver function test resul
64 ort analysis of adult patients who underwent complete blood count (CBC) and SARS-CoV-2 or influenza t
65 is per se was associated with alterations in complete blood count (CBC) and white blood cell (WBC) di
71 aged 40 to 75 years on the date of a routine complete blood count (CBC) test (index test) who had a n
72 ex (SII) were obtained from the preoperative complete blood count (CBC) test and compared between the
75 lth insurance plan who had 1 or more routine complete blood count (CBC) tests performed between Janua
76 Width (MDW), available as part of a routine complete blood count (CBC) with differential, may be a u
77 like high-performance liquid chromatography, Complete Blood Count (CBC) with peripheral smear, geneti
78 ocyte/monocyte-colony-forming unit (CFU-GM), complete blood count (CBC), and donor chimerism at vario
80 Blood samples were taken and analyzed for complete blood count (CBC), erythrocyte sedimentation ra
81 um levels of Zn, Cu, ceruloplasmin, albumin, complete blood count (CBC), fasting blood sugar (FBS), A
85 tegrated centrifugal microfluidic device for complete blood counting (CBC) has not yet been fully rea
87 investigate these differences, we evaluated complete blood counts (CBC), antibody binding of RBCs, T
89 ria were physician-ordered blood culture and complete blood count [CBC]), and 102 controls (healthy b
95 ing immune complexes, complement activation, complete blood counts, cytokine/chemokine, and gene expr
96 lection of samples of instances from routine complete blood count data in such a way that each observ
97 co-infections with dengue virus, one missing complete blood count data) and two participants who were
98 articipants who were non-Zika cases (missing complete blood count data) were excluded from analysis.
99 .g., MCP-counter, xCell, EPIC, quanTIseq) to complete blood count data, the current gold standard in
100 a standard battery of 18 biochemical tests, complete blood counts, disease complications, duration o
101 monary artery catheter insertions; number of complete blood counts, electrolytes, and cultures sent f
103 valuation regardless of the type of uveitis (complete blood count, erythrocyte sedimentation rate, C-
105 The patient underwent serial measurements of complete blood count, hepatic profile, coagulation profi
106 Of those, 9,061 users also self-reported complete blood count Hgb levels for comparison, resultin
107 cute clinical findings (signs, symptoms, and complete blood counts) in both Zika cases and non-Zika c
111 s in the immunized macaques, as indicated by complete blood counts, leukocyte differentials and hepat
115 that age-specific likelihood values for the complete blood count may determine risk of infection.
117 rn, number of patients with various abnormal complete blood count measurements, and location-specific
118 rs are adaptively identified using recurrent complete blood count measurements, which sufficiently co
119 ngs of routine laboratory testing, including complete blood count, metabolic panel with electrolytes,
120 ults of routine laboratory workup, including complete blood count, metabolic panel, and high-sensitiv
121 nts identified as having coexistent disease, complete blood counts, multiphasic biochemical testing,
124 lished that gammaP-122-I affects neither the complete blood count nor biochemical tests of liver and
125 labeling efficiency, in vitro stability, or complete blood count of leukocytes labeled with stabiliz
127 ts of Star:Star-mPEG/antimiR-145 with serial complete blood counts of leukocytes and serum metabolic
128 IFN-alpha, liver and kidney function tests, complete blood counts, or pathology of major organs are
129 y analysis revealed that, except for anemia, complete blood count parameters were within normal limit
130 for ID assessments, save time and cost using complete blood count parameters, while standardizing int
132 We included people 30 years or older with complete blood counts performed in usual clinical care a
133 5,231 individuals in the cohort, 154,179 had complete blood counts performed under acute conditions a
136 but all other laboratory findings, including complete blood count, renal function, liver function, vi
137 but all other laboratory findings, including complete blood count, renal function, liver function, vi
143 nical examination, routine laboratory tests (complete blood count, serum creatinine level), urine alb
144 included: a) the tests to be obtained daily: complete blood count, serum electrolytes, urea nitrogen,
147 use of the improved survival was unclear, as complete blood counts, splenic and marrow cellularity, n
148 resulted in significant weight loss and the complete blood count suggested the development of anemia
149 ied by para-phenylenediamine staining, and a complete blood count system was used to measure the numb
151 th negligible/negative (< 1%) yield included complete blood counts (therapy-related leukemia), dipsti
152 ecent rejection episode, cyclosporine level, complete blood count, time between transplantation and o
153 ated with BTNPs showed better restoration of complete blood count to normal level, and significantly
155 24 children with SCA with a neurologic exam, complete blood count, transcranial Doppler ultrasound (T
156 ical history and laboratory tests, including complete blood count, transferrin saturation, and other
160 ed at 1 and 3 h after preparation, whereas a complete blood count was obtained at 3 h after preparati
174 stem cell transplantation, peripheral blood complete blood counts were performed and examined for po
176 luding biochemistry, electrolyte levels, and complete blood count, were all within normal limits, exc
177 luding biochemistry, electrolyte levels, and complete blood count, were all within normal limits, exc
179 taken at baseline and at study completion; a complete blood count with differential and comprehensive
180 At endpoint, whole blood was assessed via a complete blood count with differential and immunophenoty
182 a thorough history and physical examination, complete blood count with differential, chest x-ray, uri
185 (eg, hematocrit), available in an outpatient complete blood count without differential, would be usef