Rockefeller University Press

Table I

Vascular Tumors Induced by PymT Virus and Establishment of End. Cell Lines

Tumors				End. cell lines
Genotype	Latency	Penetrance	Name	Abbr.	Origin
	d
wt+/+	8–10	29/30	bEnd.1	b1	brain
			eEnd.2	e2	yolk sac
			mEnd.3	m3	mesentery
			sEnd.1	s1	skin
			sEnd.2	s2	skin thorax
uPA−/−	10–13	9/10	mEnd.u23	u23	mesentery
			sEnd.u24	u24	skin thorax
tPA−/−	11–13	8/8	mEnd.t37	t37	mesentery
			pEnd.t38	t38	pancreas
uPA−/− tPA−/−	12–14	11/11	sEnd.ut1	ut1	skin sternum
			liEnd.ut2	ut2	liver
PAI-1−/−	6–8	3/3	luEnd.p1	p1	lung
			liEnd.p3	p3	liver
Plg−/−	8–12	9/9	ND

Tumors				End. cell lines
Genotype	Latency	Penetrance	Name	Abbr.	Origin
	d
wt+/+	8–10	29/30	bEnd.1	b1	brain
			eEnd.2	e2	yolk sac
			mEnd.3	m3	mesentery
			sEnd.1	s1	skin
			sEnd.2	s2	skin thorax
uPA−/−	10–13	9/10	mEnd.u23	u23	mesentery
			sEnd.u24	u24	skin thorax
tPA−/−	11–13	8/8	mEnd.t37	t37	mesentery
			pEnd.t38	t38	pancreas
uPA−/− tPA−/−	12–14	11/11	sEnd.ut1	ut1	skin sternum
			liEnd.ut2	ut2	liver
PAI-1−/−	6–8	3/3	luEnd.p1	p1	lung
			liEnd.p3	p3	liver
Plg−/−	8–12	9/9	ND

Supernatants from PymT-producing fibroblasts were injected into newborn wild-type and mutant mice, which were propagated by brother–sister matings. All mutant End. cell lines were established from C57Bl/6 × 129 mice. The derivation of the wild-type End. cell lines was previously described; for details regarding establishment, see Materials and Methods.

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