PMID-sentid	Pub_year	Sent_text		comp_official_name	comp_offsetprotein_name	organism	prot_offset
1322161-0	1992	Low sodium intake enhances sensitivity of 11-deoxycortisol and deoxycorticosterone to ACTH in ACTH-suppressed normal subjects.	Desoxycorticosterone	63-82	proopiomelanocortin	Homo sapiens	86-90	
1322161-0	1992	Low sodium intake enhances sensitivity of 11-deoxycortisol and deoxycorticosterone to ACTH in ACTH-suppressed normal subjects.	Desoxycorticosterone	63-82	proopiomelanocortin	Homo sapiens	94-98	
2166067-1	1990	Short term suppression of ACTH by dexamethasone effects limited reduction in plasma deoxycorticosterone (DOC) while cortisol levels are almost completely suppressed in normal control subjects.	Desoxycorticosterone	84-103	proopiomelanocortin	Homo sapiens	26-30	
1531483-7	1992	An increase in deoxycorticosterone was observed after fadrozole treatment compared with pretreatment values (P less than 0.01) and after stimulation with ACTH compared with placebo (P less than 0.05).	Desoxycorticosterone	15-34	proopiomelanocortin	Homo sapiens	154-158	
2166067-1	1990	Short term suppression of ACTH by dexamethasone effects limited reduction in plasma deoxycorticosterone (DOC) while cortisol levels are almost completely suppressed in normal control subjects.	Desoxycorticosterone	105-108	proopiomelanocortin	Homo sapiens	26-30	
35263051-3	2022	We highlight the presence of a "mineralocorticoid (MC) pathway of zona fasciculata (ZF)", where most circulating corticosterone and deoxycorticosterone (DOC) originate together with 18OHDOC, under ACTH control, a claim based on functional studies in normal subjects and in patients with 11beta-, and 17alpha-hydroxylase deficiencies.	Desoxycorticosterone	132-151	proopiomelanocortin	Homo sapiens	197-201	
34483146-10	2022	Rapid ACTH injection resulted in elevations in the deoxycorticosterone, corticosterone, aldosterone, and 17-hydroxypregnenolone levels, but not in the cortisol level.	Desoxycorticosterone	51-70	proopiomelanocortin	Homo sapiens	6-10	
35263051-3	2022	We highlight the presence of a "mineralocorticoid (MC) pathway of zona fasciculata (ZF)", where most circulating corticosterone and deoxycorticosterone (DOC) originate together with 18OHDOC, under ACTH control, a claim based on functional studies in normal subjects and in patients with 11beta-, and 17alpha-hydroxylase deficiencies.	Desoxycorticosterone	153-156	proopiomelanocortin	Homo sapiens	197-201	
7056849-3	1982	The blocking effect of met-enkephalin on the rate of aldosterone, deoxycorticosterone, and corticosterone release was significant at a concentration as low as 10(-11) M (P less than 0.001, P less than 0.01, and P less than 0.001, respectively).	Desoxycorticosterone	66-85	proopiomelanocortin	Homo sapiens	23-37	
3023428-4	1987	The episodes were caused by mineralocorticoid actions of large ACTH-induced increases in cortisol and deoxycorticosterone secretion.	Desoxycorticosterone	102-121	proopiomelanocortin	Homo sapiens	63-67	
3034556-6	1986	Plasma deoxycorticosterone (DOC), B and 18-OH-B as well as cortisol remarkable increased after ACTH injection, but the increase in plasma ALD was very small.	Desoxycorticosterone	7-26	proopiomelanocortin	Homo sapiens	95-99	
3034556-6	1986	Plasma deoxycorticosterone (DOC), B and 18-OH-B as well as cortisol remarkable increased after ACTH injection, but the increase in plasma ALD was very small.	Desoxycorticosterone	28-31	proopiomelanocortin	Homo sapiens	95-99	
3015796-8	1986	Infusion of adrenocorticotropic hormone (ACTH) caused exaggerated increases of aldosterone, 11-deoxycorticosterone, and 18-hydroxycortisol; cortisol response was normal.	Desoxycorticosterone	92-114	proopiomelanocortin	Homo sapiens	12-39	
2982239-7	1985	The fasciculata steroids cortisol, 11-deoxycorticosterone and corticosterone were continuously stimulated by ACTH.	Desoxycorticosterone	35-57	proopiomelanocortin	Homo sapiens	109-113	
6328122-0	1984	ACTH sensitivity of isolated human pathological adrenocortical cells: variability of responses in aldosterone, corticosterone, deoxycorticosterone and cortisol production.	Desoxycorticosterone	127-146	proopiomelanocortin	Homo sapiens	0-4	
6325055-2	1984	ACTH administration produced hypokalaemia, initial urinary sodium retention, a fall in active plasma renin concentration, a transient rise in plasma aldosterone concentration and sustained rises in plasma deoxycorticosterone concentration and urinary kallikrein activity.	Desoxycorticosterone	205-224	proopiomelanocortin	Homo sapiens	0-4	
6325055-4	1984	The effects of ACTH on urinary kallikrein excretion appeared to be independent of aldosterone and correlated most closely with deoxycorticosterone concentrations.	Desoxycorticosterone	127-146	proopiomelanocortin	Homo sapiens	15-19	
7056849-4	1982	Dose-dependent inhibition of steroid biosynthesis became more apparent with increasing amounts of met-enkephalin in the incubation medium (10(-11)-10(-5) M); at a concentration of 10(-5) M, met-enkephalin decreased the production of aldosterone by 45%, that of deoxycorticosterone by 51%, and that of corticosterone by 44%.	Desoxycorticosterone	261-280	proopiomelanocortin	Homo sapiens	98-112	
7056849-6	1982	In a concentration of 10(-5) M, met-enkephalin produced significant decreases in aldosterone (P less than 0.001), deoxycorticosterone (P less than 0.05), and corticosterone (P less than 0.001) production compared to the peak values obtained after stimulation with 0.85 X 10(-10) M ACTH-(1-24).	Desoxycorticosterone	114-133	proopiomelanocortin	Homo sapiens	32-46	
6291816-3	1982	Few peaks of ACTH and cortisol were simultaneous and rare secretory impulses of corticosterone, and deoxycorticosterone were in synchrony with those of ACTH or cortisol.	Desoxycorticosterone	100-119	proopiomelanocortin	Homo sapiens	13-17	
6291816-7	1982	appear to be essential in order to distinguish pituitary-dependent Cushing"s syndrome from normal; 2) In conditions of ACTH excess, DOC and corticosterone secretion seems to become progressively less ACTH-dependent as we proceed down the biosynthetic chain towards aldosterone, which is suppressed in most cases.	Desoxycorticosterone	132-135	proopiomelanocortin	Homo sapiens	119-123	
6257748-3	1981	Plasma 18-OH-DOC and B demonstrated quantitatively the greatest responses to ACTH, while DOC and 18-OHB responses were intermediate.	Desoxycorticosterone	13-16	proopiomelanocortin	Homo sapiens	77-81	
6303639-6	1983	Plasma cortisol, 11-deoxycortisol, corticosterone, deoxycorticosterone, 17 alpha-hydroxyprogesterone and 17-hydroxy, 20-dihydroprogesterone were all increased by ACTH treatment.	Desoxycorticosterone	51-70	proopiomelanocortin	Homo sapiens	162-166	
6274570-12	1981	ACTH produced increases in plasma cortisol, 11-deoxycortisol, corticosterone, deoxycorticosterone, aldosterone, 17 alpha-hydroxyprogesterone and 17 alpha,20 alpha-dihydroxyprogesterone.	Desoxycorticosterone	78-97	proopiomelanocortin	Homo sapiens	0-4	
6267148-5	1981	Plasma levels of steroids distal to progesterone, i.e., DOC, corticosterone, 18 OH-B, and aldosterone, are relatively higher after small amounts of ACTH in patients with adenomas than in normal subjects or those with adrenal hyperplasia.	Desoxycorticosterone	56-59	proopiomelanocortin	Homo sapiens	148-152	
7409273-3	1980	DOC and cortisol which were contained in the adenomas were also stimulated more significantly by ACTH than by angiotensin II and III.	Desoxycorticosterone	0-3	proopiomelanocortin	Homo sapiens	97-101	
7354720-6	1980	Correlations of free DOC and aldosterone excretion with free cortisol excretion, and their responses to the administration of metyrapone and dexamethasone were compatible with ACTH dependency in adrenal hyperplasia, autonomous production of steroids in adrenal adenomas and a chaotic steroidogenesis in adrenal carcinoma.	Desoxycorticosterone	21-24	proopiomelanocortin	Homo sapiens	176-180	
6259660-1	1980	Chronic oversecretion of adrenocorticotropin (ACTH) in Cushing"s disease and partial adrenal insufficiency results in a plasma pattern of mineralocorticoid hormones (MCHs) in which deoxycorticosterone, 18-hydroxycorticosterone and aldosterone remain within normal limits.	Desoxycorticosterone	181-200	proopiomelanocortin	Homo sapiens	46-50	
232023-2	1979	Adrenocorticotropin (ACTH)-induced steroidogenesis, obtained by continuous administration of ACTH for 3 days, produces in man (a) sustained elevations of plasma deoxycorticosterone and cortisol concentrations, (b) transient elevations of plasma aldosterone and 18-hydroxycorticosterone concentrations that return to near-control values, and (c) brisk initial increases in plasma 18-hydroxydeoxycorticosterone and corticosterone concentrations that fall to 20-68% of peak values 30 h thereafter.	Desoxycorticosterone	161-180	proopiomelanocortin	Homo sapiens	21-25	
232023-2	1979	Adrenocorticotropin (ACTH)-induced steroidogenesis, obtained by continuous administration of ACTH for 3 days, produces in man (a) sustained elevations of plasma deoxycorticosterone and cortisol concentrations, (b) transient elevations of plasma aldosterone and 18-hydroxycorticosterone concentrations that return to near-control values, and (c) brisk initial increases in plasma 18-hydroxydeoxycorticosterone and corticosterone concentrations that fall to 20-68% of peak values 30 h thereafter.	Desoxycorticosterone	161-180	proopiomelanocortin	Homo sapiens	93-97	
218456-5	1979	Since urinary tetrahydrodesoxycorticosterone increased substantially, sodium retention resulting from ACTH was ascribed to enhanced DOC secretion.	Desoxycorticosterone	132-135	proopiomelanocortin	Homo sapiens	102-106	
218456-8	1979	As a result of ACTH, plasma cortisol and the free cortisol index increased strikingly; the plasma free DOC index rose markedly in those subjects in whom the total plasma DOC level was not altered appreciably and was unchanged or even increased slightly in the few subjects in whom the total DOC level decreased.	Desoxycorticosterone	170-173	proopiomelanocortin	Homo sapiens	15-19	
218456-8	1979	As a result of ACTH, plasma cortisol and the free cortisol index increased strikingly; the plasma free DOC index rose markedly in those subjects in whom the total plasma DOC level was not altered appreciably and was unchanged or even increased slightly in the few subjects in whom the total DOC level decreased.	Desoxycorticosterone	170-173	proopiomelanocortin	Homo sapiens	15-19	
218456-9	1979	The results support the proposition that the plasma free DOC fraction is increased because of displacement from corticosteroid-binding globulin by the ACTH-induced increment in cortisol.	Desoxycorticosterone	57-60	proopiomelanocortin	Homo sapiens	151-155	
212954-9	1978	The loss of responsiveness of DOC to ACTH in the third trimester suggests that the maternal adrenals have undergone an alteration in their steroidogenic response to ACTH, but also may indicate that their output of DOC has reached a maximal rate.	Desoxycorticosterone	30-33	proopiomelanocortin	Homo sapiens	37-41	
212954-9	1978	The loss of responsiveness of DOC to ACTH in the third trimester suggests that the maternal adrenals have undergone an alteration in their steroidogenic response to ACTH, but also may indicate that their output of DOC has reached a maximal rate.	Desoxycorticosterone	30-33	proopiomelanocortin	Homo sapiens	165-169	
212954-9	1978	The loss of responsiveness of DOC to ACTH in the third trimester suggests that the maternal adrenals have undergone an alteration in their steroidogenic response to ACTH, but also may indicate that their output of DOC has reached a maximal rate.	Desoxycorticosterone	214-217	proopiomelanocortin	Homo sapiens	37-41	
190252-7	1977	Estimations of adrenal 11beta-hydroxylating efficiency in response to ACTH in patients and controls by plasma steroid ratios revealed significantly lower B/DOC ratios in both low and normal renin patients compared to controls, supported by somewhat lower F/S ratios in these patients, especially those in the low renin subgroup.	Desoxycorticosterone	156-159	proopiomelanocortin	Homo sapiens	70-74	
210631-0	1977	Prevention of the ACTH-induced hypertension by deoxycorticosterone antibody ...	Desoxycorticosterone	47-66	proopiomelanocortin	Homo sapiens	18-22	
231371-4	1979	In agreement with the results in the in vivo study, the in vitro study also revealed ACTH stimulated aldosterone and deoxycorticosterone (DOC) from the adenoma more markedly than angiotensin II or III.	Desoxycorticosterone	117-136	proopiomelanocortin	Homo sapiens	85-89	
231371-4	1979	In agreement with the results in the in vivo study, the in vitro study also revealed ACTH stimulated aldosterone and deoxycorticosterone (DOC) from the adenoma more markedly than angiotensin II or III.	Desoxycorticosterone	138-141	proopiomelanocortin	Homo sapiens	85-89	
225716-4	1979	DOC (11-deoxycorticosterone) was found in saliva only during ACTH administration.	Desoxycorticosterone	0-3	proopiomelanocortin	Homo sapiens	61-65	
225716-4	1979	DOC (11-deoxycorticosterone) was found in saliva only during ACTH administration.	Desoxycorticosterone	5-27	proopiomelanocortin	Homo sapiens	61-65	
212954-3	1978	Although DOC secretion in nongravid women has been assumed to be dependent mainly on adrenocorticotropic hormone (ACTH), in a previous study of women in the third trimester of pregnancy it was found to be unresponsive to ACTH, dexamethasone, and variations in salt intake.	Desoxycorticosterone	9-12	proopiomelanocortin	Homo sapiens	85-112	
212954-3	1978	Although DOC secretion in nongravid women has been assumed to be dependent mainly on adrenocorticotropic hormone (ACTH), in a previous study of women in the third trimester of pregnancy it was found to be unresponsive to ACTH, dexamethasone, and variations in salt intake.	Desoxycorticosterone	9-12	proopiomelanocortin	Homo sapiens	114-118	
198594-8	1977	Effects of ACTH upon plasma DOC and cortisol were not inhibited by angiotenesin III analogue, but the effect of ACTH upon aldosterone was blunted slightly.	Desoxycorticosterone	28-31	proopiomelanocortin	Homo sapiens	11-15	
199474-0	1977	[Effect of ACTH on plasma renin activity, aldosterone level and deoxycorticosterone level in humans (author"s transl)].	Desoxycorticosterone	64-83	proopiomelanocortin	Homo sapiens	11-15	
187612-8	1976	These studies suggest that a steroid other than aldosterone, 18-OH-DOC, or DOC may be the cause of the ACTH-induced hypertension in this patient.	Desoxycorticosterone	67-70	proopiomelanocortin	Homo sapiens	103-107	
168695-5	1975	Serum deoxycorticosterone rose in healthy subjects upon injection of ACTH, after induction of insulin hypoglycemia and after administration of metyrapone, while the rise was absent or blunted in patients with Addison"s disease and in patients with pituitary failure.	Desoxycorticosterone	6-25	proopiomelanocortin	Homo sapiens	69-73	
28487303-4	2017	The consequent cortisol deficiency results in a compensatory increase in adrenocorticotropic hormone (ACTH) drive, which stimulates the production of deoxycorticosterone and corticosterone leading to hypertension and hypokalaemia.	Desoxycorticosterone	150-169	proopiomelanocortin	Homo sapiens	73-100	
180044-9	1976	We suggest that competitive interactions in the protein binding properties of various steroids account for the selective effect of ACTH on the MCR of aldosterone, cortisol, and DOC.	Desoxycorticosterone	177-180	proopiomelanocortin	Homo sapiens	131-135	
4336939-8	1972	In contrast, small doses of ACTH given under similar conditions never induced increases in plasma deoxycorticosterone without simultaneously inducing large increases in plasma deoxycortisol.	Desoxycorticosterone	98-117	proopiomelanocortin	Homo sapiens	28-32	
14927717-0	1952	Inhibition of desoxycorticosterone-induced pathologic changes by adrenocorticotropic hormone and cortisone.	Desoxycorticosterone	14-34	proopiomelanocortin	Homo sapiens	65-92	
28487303-4	2017	The consequent cortisol deficiency results in a compensatory increase in adrenocorticotropic hormone (ACTH) drive, which stimulates the production of deoxycorticosterone and corticosterone leading to hypertension and hypokalaemia.	Desoxycorticosterone	150-169	proopiomelanocortin	Homo sapiens	102-106	
26525354-11	2015	In infancy and childhood adrenal androgen overproduction results in peripheral precocious puberty in boys and various degrees of virilization in girls.Accumulation of 11-deoxycorticosterone and its metabolites causes hypertension in about two thirds of patients.Diagnosis lies upon elevated 11-deoxycortisol and DOC plus upstream precursors, such as 17alpha-hydroxyprogesterone and Delta4-androstenedione.The established treatment of steroid 11beta-OHD is similar to that of steroid 21-hydroxylase deficiency and consists of glucocorticoid administration in order to reduce ACTH-driven DOC overproduction resulting in hypertension remission and improvement of the virilization symptoms.	Desoxycorticosterone	167-189	proopiomelanocortin	Homo sapiens	574-578	
12040893-5	2002	Also, the therapeutic activity of ACTH in infantile spasms could partially relate to its stimulatory effects on the synthesis of DOC, which then undergoes biotransformation to neurosteroids.	Desoxycorticosterone	129-132	proopiomelanocortin	Homo sapiens	34-38	
10454460-6	1999	Plasma deoxycorticosterone levels were lower in blacks than in whites both at baseline (247+/-161 versus 381+/-270 pmol/L, P=0.048) and after stimulation with adrenocorticotropic hormone (822+/-294 versus 1127+/-628 pmol/L at 30 minutes, P=0.047; 925+/-366 versus 1440+/-834 pmol/L at 60 minutes, P=0.013).	Desoxycorticosterone	7-26	proopiomelanocortin	Homo sapiens	159-186	
1337504-13	1992	In ectopic ACTH syndrome the characteristic mineralocorticoid excess can be accounted for by a combination of increased secretion of cortisol, corticosterone and of 11-deoxycorticosterone and decreased inactivation of cortisol and corticosterone by 11 beta-dehydrogenase.	Desoxycorticosterone	165-187	proopiomelanocortin	Homo sapiens	11-15