PMID-sentid	Pub_year	Sent_text		comp_official_name	comp_offsetprotein_name	organism	prot_offset
6238856-0	1984	Attachment and phagocytosis by salmon macrophages of agarose beads coated with human C3b and C3bi.	Sepharose	53-60	endogenous retrovirus group K member 3	Homo sapiens	85-88	
2212692-3	1990	The amount of C3b immobilized by each support varied from 81% for Actigel A aldehyde activated agarose to only 19% for Reacti-Gel GF-2000.	Sepharose	95-102	endogenous retrovirus group K member 3	Homo sapiens	14-17	
2197048-10	1990	On the other hand, when GM-CSF/IL-3-activated eosinophils were exposed to known secretory stimuli, there was a six-fold increase in the amount of ECP released when the cells were stimulated with sepharose coated with C3b, and a two-fold increase when they were stimulated with sepharose-activated whole autologous serum.	Sepharose	195-204	endogenous retrovirus group K member 3	Homo sapiens	217-220	
2197048-10	1990	On the other hand, when GM-CSF/IL-3-activated eosinophils were exposed to known secretory stimuli, there was a six-fold increase in the amount of ECP released when the cells were stimulated with sepharose coated with C3b, and a two-fold increase when they were stimulated with sepharose-activated whole autologous serum.	Sepharose	277-286	endogenous retrovirus group K member 3	Homo sapiens	217-220	
4028522-2	1985	The activated form of the third component of complement, C3b, which had bound to the radioactive cysteine was then released from the agarose bead with dithiothreitol.	Sepharose	133-140	endogenous retrovirus group K member 3	Homo sapiens	57-60	
2580903-6	1985	Adsorption of detergent lysates of L929 cells with C3bgp-Sepharose depleted by 44% the antigen recognized by anti-human CR1; the C3bgp-binding protein and the cross-reactive antigen exhibited similar patterns on two-dimensional gel electrophoresis; and the isolated C3b-binding protein could be immunoprecipitated with anti-human CR1.	Sepharose	57-66	endogenous retrovirus group K member 3	Homo sapiens	51-54	
6234177-3	1984	136: 111) using radiolabeling methods, we characterized from the membrane of the human B lymphoblastoid cell line Raji, a 140 000-Mr glycoprotein (gp140) carrying a C3b-binding activity with 125I-labeled C3b or Sepharose-bound C3b.	Sepharose	211-220	endogenous retrovirus group K member 3	Homo sapiens	165-168	
8080606-2	1993	In the normal Indian population, purification of CR1 by immunoprecipitation or C3b-Sepharose affinity column and subjecting it to electrophoresis showed the existence of two types of structural polymorphic patterns with M(r) of 190 kDa and 220 kDa, and with gene frequencies of 0.975 and 0.025, respectively.	Sepharose	83-92	endogenous retrovirus group K member 3	Homo sapiens	79-82	
2786912-0	1989	Preparation of monoclonal antibodies to C3b by immunization with C3b(i)-sepharose.	Sepharose	72-81	endogenous retrovirus group K member 3	Homo sapiens	40-43	
2786912-0	1989	Preparation of monoclonal antibodies to C3b by immunization with C3b(i)-sepharose.	Sepharose	72-81	endogenous retrovirus group K member 3	Homo sapiens	65-68	
2786912-3	1989	Instead, C3b and C3bi were deposited on Sepharose 4B via the alternative pathway of complement activation in normal human serum, and this C3b(i)-Sepharose served as the immunogen.	Sepharose	40-52	endogenous retrovirus group K member 3	Homo sapiens	9-12	
2786912-3	1989	Instead, C3b and C3bi were deposited on Sepharose 4B via the alternative pathway of complement activation in normal human serum, and this C3b(i)-Sepharose served as the immunogen.	Sepharose	40-52	endogenous retrovirus group K member 3	Homo sapiens	17-20	
2786912-3	1989	Instead, C3b and C3bi were deposited on Sepharose 4B via the alternative pathway of complement activation in normal human serum, and this C3b(i)-Sepharose served as the immunogen.	Sepharose	40-49	endogenous retrovirus group K member 3	Homo sapiens	9-12	
2786912-3	1989	Instead, C3b and C3bi were deposited on Sepharose 4B via the alternative pathway of complement activation in normal human serum, and this C3b(i)-Sepharose served as the immunogen.	Sepharose	40-49	endogenous retrovirus group K member 3	Homo sapiens	17-20	
2786912-4	1989	C3b(i)-Sepharose was also prepared from a number of primate and non-primate sources, and this allowed us to demonstrate that the anti-human C3b MAbs cross-reacted with primate-derived C3b, but not with C3b from non-primates.	Sepharose	7-16	endogenous retrovirus group K member 3	Homo sapiens	0-3	
2786912-4	1989	C3b(i)-Sepharose was also prepared from a number of primate and non-primate sources, and this allowed us to demonstrate that the anti-human C3b MAbs cross-reacted with primate-derived C3b, but not with C3b from non-primates.	Sepharose	7-16	endogenous retrovirus group K member 3	Homo sapiens	140-143	
2786912-4	1989	C3b(i)-Sepharose was also prepared from a number of primate and non-primate sources, and this allowed us to demonstrate that the anti-human C3b MAbs cross-reacted with primate-derived C3b, but not with C3b from non-primates.	Sepharose	7-16	endogenous retrovirus group K member 3	Homo sapiens	140-143	
2786912-4	1989	C3b(i)-Sepharose was also prepared from a number of primate and non-primate sources, and this allowed us to demonstrate that the anti-human C3b MAbs cross-reacted with primate-derived C3b, but not with C3b from non-primates.	Sepharose	7-16	endogenous retrovirus group K member 3	Homo sapiens	140-143	
2963863-7	1988	This specificity of binding and the ability to rebind to a second column of iC3- or C3b-thiol-Sepharose are comparable to human CR1.	Sepharose	94-103	endogenous retrovirus group K member 3	Homo sapiens	84-87	
6238856-3	1984	Furthermore, agarose beads coated with human C3b and C3bi after incubation with isolated complement factors (C3, D, B), were associated to 30-40% of the phagocytes.	Sepharose	13-20	endogenous retrovirus group K member 3	Homo sapiens	45-48	
6238856-7	1984	Agarose beads coated with these ligands (C3b and C3bi) are attached and ingested by the phagocytes.	Sepharose	0-7	endogenous retrovirus group K member 3	Homo sapiens	41-44	
7056569-1	1982	C3b receptor protein was purified form human erythrocytes by 2 M KBr solubilization and affinity chromatography on C3-coated sepharose.	Sepharose	125-134	endogenous retrovirus group K member 3	Homo sapiens	0-3